Centro Cardiologico Monzino Scientific Report 2011 Ongoing Research 2012 Scientific Report 2011 Ongoing Research 2012 Chairman’s message Cardiovascular diseases and cancer remain the most frequent causes of death in the Western world and, in order to combat these diseases, our efforts have been directed toward the development of research in these important fields. Despite of the deep economic crisis that has affected Europe, and in particular our country, the clinical and research activities at the European Institute of Oncology and at Centro Cardiologico Monzino during 2011 and the first part of 2012 have had a positive trend, allowing to offer the patient the best standard of care. In order to do this, a coordinated effort to optimize the use of economical and human resources has been developed and, thanks to the tireless and passionate work of our researchers and clinicians, important advances in the care of these life-threatening pathologies have been achieved. In this context a special thank is given to our former CEO Carlo Ciani for the overall activities he carried out during the last years. Carlo BUORA Chairman CCM — Scientific Report 2011 — Ongoing research 2012 5 Contents • CEO message • Scientific Director’s Report • The Research Laboratories • Grants Office • Department of Cardiovascular Sciences • Centre of Pharmacological Research for the Study and Prevention of Cardiovascular Diseases • Directive Board • General Management • Outpatient Service and Marketing • Safety, Enviroment and Quality • Finance and Administration • Human Resources • Information & Communication Technology • Ethics Committee • Library • Educational and Training • Medical Director’s Report • Medical Directorate’s Staff • Clinical Governance at Centro Cardiologico Monzino • Cardiovascular Tissue Bank • Cardiovascular Telemedicine Colophon Title Publisher Number Month/Year Editor Authors Secretary of editing Photographer Typographer Paper CCM Scientific Report 2011. Ongoing Research 2012. CCM Centro Cardiologico Monzino©, Milan (Italy) 3 December 2012 Elena Tremoli Each Unit was in charge of the writing of its own text. Nicoletta Malgaretti, Mirko Nesurini Roberto Benzi Italgrafica (NO), Printed in Italy Printed on the uncoated paper On Offset whose elementary chlorine free pulps came from susteinaible forests CLINICAL UNITS Emergency Unit Acute Cardiac Care Unit Intensive Cardiac Care Unit Heart Failure, Clinical Cardiology and Cardiac Rehabilitation Unit Interventional Cardiology Units Electrophysiology Unit Cardiac Surgery Unit Extracorporeal Circulation Service Vascular Ultrasound Service Vascular and Endovascular Surgery Unit Anaesthesiology and Intensive Care Unit Echocardiography Unit Magnetic Resonance Imaging Unit Radiology Unit Laboratory Medicine Unit 11 13 15 18 19 21 22 23 24 25 26 27 28 29 30 31 33 42 44 48 50 54 56 58 62 68 71 74 80 81 82 84 88 90 92 96 RESEARCH LABORATORIES Laboratory of Biology and Biochemistry of Atherothrombosis 100 Unit of Cell Biology and Biochemistry of Atherothrombosis 102 Unit of Cardiovascular Proteomics 106 Unit of Biochemistry of Oxidative Stress and Endothelial Function in Atherothrombosis 112 Unit of Experimental Thrombosis and Imaging in vivo 118 Program for the Control of Global Cardiovascular Risk 121 Unit of Atherosclerosis Prevention 122 Unit of Arterial Morphology and Function 124 Unit of Biostatistics 126 Laboratory of Immunology and Functional Genomics 128 Laboratory of Vascular Biology and Regenerative Medicine 132 Laboratory of Cardiovascular Tissue Engineering 138 Plasma and Gene Bank 144 DNA Bank 144 CLINICAL RESEARCH Relationship between heart and kidney function in acute cardiovascular conditions Candidate biomarkers for the clinical and prognostic stratification of patients with acute coronary syndromes Cardiopulmonary physiopathology Interventional cardiology Electrophysiology Area: scientific hot topics Cardiovascular imaging Clinical Research on Atherothrombosis Transcatheter aortic valve implant (TAVI) Arrhythmia surgery Vascular surgery BASIC AND TRANSLATIONAL RESEARCH Prospective evaluation of platelet activation markers in patients treated with drug-eluting stents: platelet-associated Tissue Factor predicts the risk of future revascularization in a pilot study 146 148 150 154 158 165 170 178 180 184 188 Proteomics-based development of biomarkers in cardiovascular disease Red blood cells as a source of nitric oxide Heterogeneity of human macrophages in culture and in atherosclerotic plaque Experimental imaging of brain and heart ischemia Interaction between food and cardiovascular drugs Food-blood fatty acids and coronary heart disease Role of the longevity genes p66sh/sirt1 in insulinresistance, diabetes and cardiovascular disease High resolution B-mode ultrasound imaging High resolution B-mod ultrasound imaging for the assesment of mechanism involved in atherosclerosis progression New methods to analyze complex ultrasound measures and atherosclerosis progression Cardiovascular epigenetics microRNAs in cardiovascular diseases Regenerative medicine in cardiovascular diseases 190 192 194 196 199 202 204 207 212 215 219 222 224 Board of Directors As of June 2012 Carlo BUORA Carlo Ciani Mauro Melis Marco AGNELLI Stefano MICHELINI Mario Cesana Chairman Deputy Chairman Chief Executive Officer ex officio Lorenzo CAMMELLI Elena Tremoli Auditors Maurizio BOZZATO Guido CROCI Pierluigi DAVIDE PUBLICATIONS, CLINICAL RESEARCH PROJECTS, SEMINARS Full papers 229 Clinical Research Projects 234 Ongoing grants 244 Seminars, conferences and courses 248 CCM — Scientific Report 2011 — Ongoing research 2012 9 Chief Executive Officer’s Message During 2011 and the first part of 2012 Centro Cardiologico Monzino has been able to maintain and even to increase its level of excellence with a good economical performance, despite the difficulty of this time period, as outlined by dr. Buora. This means that the decision of our shareholders, who contributed to creating the Institute over the years, was an excellent one. We hope that the economical conditions will allow us in the future to carry out further investments in research and technology aimed at improving even further the effectiveness of our treatments. We are constantly engaged in clinical practice to maintain a high quality care for our patients, developing in-house and external training for many family doctors and specialists who see the Institute as a center of excellence and reference for cardiovascular diseases. Mauro MELIS Chief Executive Officer CCM — Scientific Report 2011 — Ongoing research 2012 11 Scientific Director’s Report Elena Tremoli, Ph.D Scientific Director Scientific Direction Secretariat and Grants Office: Chiara Centenaro, Maria Lucarelli, Nicoletta Malgaretti, Luisa Triglia Lab Manager: Alessandra Terragni Elena TREMOLI, Ph.D Scientific Director Centro Cardiologico Monzino is the only Institute of excellence all over Europe exclusively devoted to cardiovascular diseases. Our mission is to understand the underlying causes of the diseases of the heart and the vascular tree and to develop new treatments and cures for our patients. Within this frame the Scientific Direction provides planning, directions, and support to the different components of the Institute. Indeed, “the patient” is central in all our activities and everybody’s efforts are directed towards the strategic objectives of the Institute in order to create the best conditions to allow operators and medical staff to put their knowledge to patients’ service and our Scientific and Management Boards to guarantee that the everyday activity reflects these basic principles. In July 2011, after more than one decade of Scientific Direction, prof. Paolo Biglioli retired and prof. Elena Tremoli has taken the responsibility of the Scientific Direction of Centro Cardiologico Monzino. Since then, a number of activities have been carried out both in basic and clinical research in order to strengthen the scientific exchanges between cardiologists, heart and vascular surgeons and basic researchers, with the aim to further implement the translational feature of the research and ultimately to develop a full model of translational medicine to be applied to Centro Cardiologico Monzino. The implementation of collaborations among different scientific disciplines and through activities that will provide to scientists and clinicians a fostering ground for their scientific work, has been among the jobs developed during this year. In addition the Scientific Direction is working in monitoring and analysing industrial trends in pertinent areas in order to facilitate the development of new research projects, which may ultimately result in strengthening the relationship between public authorities and enterprises both at Italian and European level. Centro Cardiologico Monzino project leaders provide a strategic focus in establishing the critical path needed to move the research down the translational path, helping to form project teams, bridging information across disciplines, ensuring high quality data systems and providing funding, also through the identification of additional resources. Many new clinical projects started during the year, soon after the approval of the Scientific and Ethics Committees. We also had a consistent number of visitors from all part of the world attending the research laboratories and the clinical Units. Training of young scientists and physicians is part of our mission. Many members of our staff were actively involved in courses, seminars and conferences both for external and internal attendance. We developed collaborations with several European countries, and specific efforts were devoted to establish contacts and cultural relationships with new cardiovascular centres. Overall, 2011 has been a fruitful year for publications, since the total impact factor has increased with respect to 2010. The scientific production, in terms of papers published on peer-reviewed journals, is all centred in the cardiovascular field spanning from clinical and interventional cardiology, to heart and vascular surgery, with a focus on new imaging techniques to visualize the heart and the vascular tree and on the development of biomarkers for the identification of patients at high risk to develop the first (primary prevention) or further (secondary prevention) cardiovascular events. Special focus has been given, as before, to education. During this year the Department of Cardiovascular Sciences of the University of Milano has been merged with other Institutes to create the Department of Clinical Sciences and Community Health. Centro Cardiologico Monzino hosts the Cardiovascular Section of this Department, chaired by Prof. Cesare Fiorentini. In addition, the Postgraduate School CCM — Scientific Report 2011 — Ongoing research 2012 13 The Research Laboratories in Heart Surgery, chaired by Prof. Alamanni, the Postgraduate School in Cardiology, chaired by prof. Fiorentini, the first level Degree in Techniques of Cardiocirculatory Pathophysiology and the Master in Cardiovascular Nursing are based in the Institute. Finally, Centro Cardiologico Monzino hosts the Centre of Pharmacological Research for the Study and Prevention of Cardiovascular Diseases of the University of Milano. In conclusion, 2011 was a productive year, full of positive news even though we had to deal with a severe economic crisis and a rationalization of costs and expenses in the research activities. Nevertheless, thanks to the help of everybody, Centro Cardiologico Monzino has been active and successful in terms both of scientific goals achieved, and, most importantly, of clinical results in the care of patients affected by cardiovascular diseases. Publications 2000 — 2011 2000 2001 2002 2003 2004 2005 2006 2007 2008 2009 2010 2011 29 26 42 41 50 56 68 98 63 76 111 114 Full Papers Journal with Impact Factor Total Impact Factor (*) 89,47 77,92 199,34 227,86 258,798 326,05 488,215 466,974 309,841 559,95 647,97 672,02 Average Impact factor 3,09 3,00 4,86 5,56 5,18 5,82 7,18 4,77 4,92 6,51 5,84 5,89 Full Papers Journal without Impact factor 8 11 19 16 10 18 8 14 15 24 16 16 Total Full Paper 37 37 60 57 60 74 76 112 78 100 127 130 (*) For each year the IF was calculated using values published in the Journal Citation Reports of the previous year 14 CCM — Scientific Report 2011 — Ongoing research 2012 During 2011 Centro Cardiologico Monzino has carried out translational research focused on the study of cardiovascular disease. A global approach to this field has been used taking advantage from the new -omics, e.g. genomic and proteomic, and other innovative technologies to the emerging problems in cardiology and heart and vascular surgery. This has allowed the quick translation of emerging scientific knowledge into new strategies for the prevention and treatment of cardiovascular diseases. The four major basic research programs (Biology and Biochemistry of Atherothrombosis, Vascular Biology and Regenerative Medicine, Immunology and Functional Genomics, Cardiovascular Tissue Engineering) operate in strict conjunction with the clinical and surgical Units of Centro Cardiologico Monzino. The program of the Laboratory of Biology and Biochemistry of Atherothrombosis is focused on the studies of both the vessel wall and circulating cells, with a major focus on the study of platelet biochemistry and function in patients with atherothrombosis and/or coronary disease. The Laboratory of Vascular Biology and Regenerative Medicine is exploring the potential of the cellular cell therapy in cardiovascular disease, with the aim to increase its potential. The Laboratory of Immunology and Functional Genomics focuses on the investigation of the immunological events associated with the formation of atherosclerotic plaque and the occurrence of thrombus in cardiovascular diseases. Functional genomics goals of this laboratory include studies on gene expression and control, investigation of mutations that cause function loss or alteration, and development of experimental and computational methods for protein analyses. Researches involving genetically modified animal models as well as new experimental imaging approaches are also carried out. The mission of the Laboratory of Cardiovascular Tissue Engineering is to devise strategies to derive a new generation of cardiovascular implants and devices, by combining cardiovascular stem cell knowledge and material/biomechanics expertise. Starting from basic investigations on human-derived cardiovascular progenitors such as cord blood-/peripheral blood-/ bone marrow-derived endothelial progenitor cells (EPCs), cardiac resident stem cells (CSCs), saphenous vein progenitors (SVPs) and the so called aortic valve interstitial cells (VICs), the mechanisms linked to physiologic or pathologic differentiation of these cells is being studied by application of “high content” molecular analysis and high throughput material screening methods allowing a rapid search for novel bio-materials (polymers, hydrogels and biological scaffolds) to embed stem cells in culture. Particularly relevant appears, in this scenario, also the investigation on strain- and mechanical stress-associated stem cells response Moreover, a Program for the Control of Global Cardiovascular Risk is ongoing. Lifestyle and pharmacological approaches are applied to patients’ CCM — Scientific Report 2011 — Ongoing research 2012 15 treatment in order to reduce their cardiovascular risk. At Centro Cardiologico Monzino five major lines of clinical research are ongoing: • Critical cardiology • Interventional cardiology • Electrophysiology • Cardiac and Vascular Surgery • Imaging And research is carried out in the following laboratories: • Heart and vascular surgery • Anaesthesiology • Cardiovascular Imaging • Electrophysiology • Clinical Laboratory Medicine Many new clinical projects started during the year, soon after the approval of the Scientific and Ethics Committees. We also had a consistent number of 16 CCM — Scientific Report 2011 — Ongoing research 2012 visitors from all part of the world attending the research laboratories and the clinical Units. Training of young scientists and physicians is part of our mission. Many members of our staff were actively involved in the Department and Postgraduate Schools of the Milano University and were engaged in teaching and lecturing at scientific meetings. Numerous meetings were organized by Centro Cardiologico Monzino, both for external and internal attendance. We developed collaborations with several European countries, and specific efforts were devoted to establish contacts and cultural relationships with new cardiovascular centres in Saudi Arabia, Libya and Arab Emirates. Thanks to national and international funds, we were successful in supporting research activities. We expect to further increase our fund raising capacity and are very grateful to all granting agencies that recognized the validity of our projects. The Scientific Director and the Directors of the Research Laboratories: Maurizio Capogrossi, Elena Tremoli, Gualtiero Colombo, Gianluca Polvani. CCM — Scientific Report 2011 — Ongoing research 2012 17 Grants Office University Department of Cardiovascular Sciences Cesare FIORENTINI, Full Professor Director Within the Scientific Direction, the Grants Office acts as a link between researchers and sponsoring agencies and is a central source of information on major national and international agencies, foundations, and institutions that support research and scholarships. It assists researchers in identifying appropriate research funding opportunities providing support in the preparations of applications, developing proposal narratives and budgets, completing the application forms and interpreting the regulations of the granting agencies, assuring compliance with the sponsor’s policies and requirements. It negotiates the terms and conditions of awards, of successful proposals and provides support for the administration of research grants, including funding allocation, monitoring research expenditures and producing financial statements. It manages research contracts, preparing, whenever necessary, subcontracts or consortium agreements with collaborating institutions and provides administrative support for Centro Cardiologico Monzino. 18 CCM — Scientific Report 2011 — Ongoing research 2012 Vice Director: Francesco ALAMANNI, Full Professor STAFF University: Piergiuseppe Agostoni, Assoociate Professor, Marco Agrifoglio, Associate Professor, Vincenzo Arena, Assistant Professor, Antonio Bartorelli, Associate Professor, Viviana Cavalca, Assistant Professor, Francesco Donatelli, Full Professor, Luisa Gregorini Ventura, Associate Professor, Alessandro Lualdi, Assistant Professor, Piero Montorsi, Associate Professor, Alessandro Parolari, Assistant Professor, Marco Pocar, Assistant Professor, Gianluca Polvani, Full Professor, Giulio Pompilio, Assistant Professor Administrative: Francesco Barresi, Eleonora Boccato, Loredana Boccotti, Anna Cerini, Alessandro Gabrieli Cardiology Fellows: Laura Antonioli, Francesca Baratto, Stefano Bartoletti, Daniela Benedetto, Erika Bertella, Filippo Billi, Costanza Boiti, Angelo Cabiati, Chiara Colombo, Sarah Cortinovis, Maria Antonietta Dessanai, Anna Garlaschè, Pamela Gatto, Sarah Ghulam Ali, Giuliano Giusti, Erica Gondoni, Monica Sonia Loguercio, Massimo Mapelli, Andrea Marinetti, Lucia Mauri, Valentina Milazzo, Marco Valerio Morpurgo, Saima Mushtaq, Paolo Olivares, Chiara Stefania Pandini, Margherita Pirondini, Francesca Pizzamiglio, Ilaria Previtali, Mara Rubino, Laura Salvini, Chiara Segurini, Marco Vicenzi , Carlo Vignati Heart Surgery Fellows: Francesco Arlati, Cristina Borsetti, Laura Cavallotti, Alberto Clerici, Monica Contino, Puma Dennis Ezra Cusihuaman, Andrea Daprati, Tommaso Generali, Sara Filippini, Marco Gennari, Daniela Manzone, Elisa Merati, Nuri Halkawt Ali Nuri, Davide Patrini, Alberto Pilozzi Casado, Camillo Poloni, Gabriele Tamagnini, Giulio Tessitore Centro Cardiologico Monzino was founded by cavalier Italo Monzino and professor Cesare Bartorelli in 1981 with the aim to develop cardiology in Italy. As the result of cooperation between the Milano University and a private foundation, Centro Cardiologico Monzino became a monothematic hospital, home of many academic activities. Since then, the Centre has been hosting university competences in cardiovascular field, both clinical and surgical. University cardiologists and heart surgeons all belong to the Department of Cardiovascular Sciences, School of Medicine and Surgery, Milano University. At present several University programs are ongoing: Degree in Medicine and Surgery, Postgraduate School in Cardiology, Postgraduate School in Heart Surgery, First Level Degree in Techniques of Cardiocirculatory Pathophysiology, Master in Cardiovascular Nursing, Master in Cardiac and Ultrasound Techniques, Advanced Training Course in Electrocardiography, Arrhythmology and Advanced Life Support. The staff of the Department of Cardiovascular Sciences carries out research activity in strict collaboration with the staff of Centro Cardiologico Monzino. CCM — Scientific Report 2011 — Ongoing research 2012 19 University Centre of Pharmacological Research for the Study and Prevention of Cardiovascular Diseases It should be noted that, as part of the university departmental reorganization (Law Gelmini 240/2010, December 2010), during year 2012 the Department of Cardiovascular Sciences will be joined to other departments of the Milano University to set up the wider Department of Clinical Sciences and Community Health. As provided by the renewed Charter of the Milano University, the Department of Cardiovascular Sciences will constitute the Section of Cardiovascular Sciences, which continues to be based at Centro Cardiologico Monzino. Elena TREMOLI, Full Professor Director Scientific Committee: Mariapia Abbracchio, Full Professor, Francesco Alamanni, Full Professor, Damiano Baldassarre, Assistant Professor, Marina Camera, Assistant Professor, Donatella Caruso, Associate Professor, Susanna Colli, Associate Professor, Alberto Corsini, Full Professor, Giancarlo Folco, Full Professor, Alessandro Lualdi, Assistant Professor, Rodolfo Paoletti, Full Professor, Alessandro Parolari, Assistant Professor, Gianluca Polvani, Full Professor, Giulio Pompilio, Assistant Professor, Angelo Sala, Associate Professor, Cesare Sirtori, Full Professor, Mauro Amato, Carlo Ciani, Gianni Giorgi, Pablo Werba The activity of the Centre is focused on the study and prevention of cardiovascular diseases and, with the support of external collaborations, aims at developing basic research on cellular biology and biochemistry of atherosclerosis and thrombosis in patients affected by cardiovascular diseases. A further aim is to evaluate the efficacy of pharmacological interventions in the cure and prevention of patients undergoing surgical heart revascularization. Activities • Program for primary and secondary prevention of cardiovascular diseases • Research programs /projects in collaboration with other Italian Atherosclerosis Centres • Scientific communication /scientific activity communication • Masters and specializing courses • Seminars, congresses, meetings with experts • Grants for young researchers 20 CCM — Scientific Report 2011 — Ongoing research 2012 CCM — Scientific Report 2011 — Ongoing research 2012 21 General Management The mission of the Centro Cardiologico Monzino Management is to favour patient care, creating the best conditions to allow the operators to put their expertise and knowledge to the patients’ service. In a complex organization there are many ways to play this role, but we believe that our managers must necessarily own the following principles: Stefano MICHELINI General Manager Directive Board Chief Executive Officer Mauro Melis General Manager Stefano Michelini Chief Financial Officer Mario Cesana Management Director Enrico Parma Chief Human Resources Officer Daniele Piacentini Chief Information Officer Claudio Carlo Franzoni Medical Director Lorenzo Cammelli Scientific Director Elena Tremoli Cardiology Program Director Cesare Fiorentini 22 CCM — Scientific Report 2011 — Ongoing research 2012 General Manager’s Assistant: Graziella Bassanello Area Coordinators: • Critical Cardiology • Cardiovascular Surgery • Interventional Cardiology • Cardiovascular Imaging • Electrophysiology Piergiuseppe Agostoni Francesco Alamanni Antonio Bartorelli Mauro Pepi Claudio Tondo Unit Directors: • Cardiovascular Surgery 2 • Intensive Care Gianluca Polvani Erminio Sisillo • a continuous stimulus towards innovation and international dimension with the belief that a research institute can only excel if it is based on mature and advanced management tools • a team culture to be searched for and promoted every day in the relationships with all those who operate inside the Institute • the awareness that, in such no-profit organizations as Centro Cardiologico Monzino, the Management systems justify their existence inasmuch as they strongly contribute to create the conditions to reach and maintain excellence in the cardiovascular field This is, in synthesis, the philosophy that guides the behaviour of the areas that coordinate and support Centro Cardiologico Monzino clinical and research activities. Our job, our active contribution to the fight against cardiovascular diseases, is to try and to put into practice this “philosophy”. CCM — Scientific Report 2011 — Ongoing research 2012 23 Outpatient Service and Marketing Safety, Enviroment and Quality Enrico Parma Management Director Fabio Tealdi Chief Safety, Enviroment and Quality Officer STAFF Management Director’s Assistant: Fannina Manzella Outpatient Service Manager: Fabio Tealdi Private Admittance: Raffaella Graticoli Marketing, Events and Internet: Alfredo Pascali Content Manager and Scientific Writer: Andreina Folli The outpatient service manages the accessibility of the clinical paths for outpatients ensuring appropriate administrative, clinic and logistic admittance. Planning and implementation of visits and diagnostics are included as well as the invoicing process to public and private companies. • Booking management through Call Center, Front lines, Internet • Admittance front lines • Clinical records services • Service Planning • Management of data flows and invoicing The Marketing Team of the Centro Cardiologico Monzino, in close collaboration with the IEO Marketing Team, is involved in many organisational aspects (sales and promotion, market development, internet, events) and supports communication, fund raising, branding and press so that group standards are efficiently applied to the cardiovascular field. The Team facilitates the organization of conferences, seminars and events and in particular is involved in the planning of the “World Heart Day”, usually held on the last week of September, a successful traditional event attracting hundreds of people interested in cardiovascular prevention. In addition, the Team takes care of the development and updating of the web site (www.cardiologicomonzino.it) to further expand the Centro Cardiologico Monzino virtual community. An Alumni section has been created as well as blogs, App and links to the main social networks. The Marketing Team is in charge of the commercial relationships with the private health insurance and founds sector and the setting of the fee schedule. 24 CCM — Scientific Report 2011 — Ongoing research 2012 Quality Management is pursued in order to basically ensure safety of the patients and quality of care with reference to the JCI scheme, to the ISO9001 standard and to the requirements of the national and regional laws. The Management of Quality includes the handling and follow up of complaints for both outpatients and inpatients and customer satisfaction reviews. Environmental requirements are satisfied ensuring compliance to the relevant laws (Dlgs152/2006) and with a management system that follows the BS14001 standard. Safety of the workplace is ensured through a management system that complies with the provisions of the standard OHSAS18001 and with reference to the laws (Dlgs81/08 and related requirements) CCM — Scientific Report 2011 — Ongoing research 2012 25 Finance and Administration Human Resources Mario Cesana Chief Financial Officer Daniele Piacentini Chief HR Officer STAFF Financial and Accounting Office: Riccardo Quintini Purchasing Office and Technical Service: Gianfranco Piantelli Management Control and Budgeting: Enrico Parma (ad interim) Integration of the clinical, research and administrative areas represents the basic principle underlying the management model adopted by the Finance and Administration Management. The main tasks of the Financial Management are as follows: • Optimization of entire diagnostic, treatment and administrative path of each patient • Economic - financial management of the Institute • Administrative, legal and tax requirements • Managing the accounting, procurement and stock Human Resources & Education: Federica Vaga The central role of the individual and top-quality assistance are the two principles that have always inspired the organizational and management work done by the HR Office in each of the above areas. These principles have enabled the Institute to achieve its main objective: improving the quality of life of each patient, who must be considered not simply as a person who needs treatment, but, above all, as a multifaceted human being. Main tasks of the HR Office are as follow: • recruitment and selection • education and training • performance evaluations • salary packages and incentives • personnel management, planning and costs • union relations • work organization The HR Office is in charge of the following services: • Performance management & organization • Pay Roll Office • Recruitment • Education and training 26 CCM — Scientific Report 2011 — Ongoing research 2012 CCM — Scientific Report 2011 — Ongoing research 2012 27 Information & Communication Technology Ethics Committee Claudio Carlo Franzoni Chief Information Officer STAFF Business Applications: Paolo Zilioli Research Area: Alessandro Dellavedova Clinical Area: Luigi Grilli Governance: Luigi Cassi Innovation and Technologies: Alberto Mancin The ICT Department handles the whole computing infrastructure: maintenance and support of Office Automation, management of network infrastructure and telephony, design and development of new applications. The main tasks of the ICT Department are as fellows: • management, maintenance and updating of third party applications, providing user support • design and development of applications to enable clinical and administrative process execution • design, development and management of the network infrastructure, servers and telephony • design, development and management of the software and the basic application services • management of the structure, organization and content of data • management of the safety and security of data and resources • technical and usage support on Information Services • providing computer hardware and software technical support • defining products and technology standards and research innovative solutions The ICT Department is in charge of the following services: • Development and Programming • Networks and Systems • Information Systems and Research 28 CCM — Scientific Report 2011 — Ongoing research 2012 Giuseppe FOLLI Chairman ferruccio BERTI Vice Chairman Atanasio NONIS Secretary Giuseppe Arosio Maria Santina Bonardi Lorenzo Cammelli Giorgio Dazzo Susanna Dellepiane Antonio Liverani Maurizio Pellegrini Elena Tremoli Emanuela Valaguzza SECRETARIAT Daniela TAMAGNI OBSERVERS Mauro Melis Stefano MICHELINI A central role in the clinical research of the Centro Cardiologico Monzino is played by its Ethics Committee. The scientific aspects, the expected improvements in the general health and well being and the overall riskbenefit ratio of the participants are the milestones of the evaluation work carried out by the Ethics Committee which covers the whole range of clinical research projects, involving the evaluation of medicinal products, devices, other interventional techniques as well as observational studies. The Committee is accredited at the Ministry of Health, the National Drug Agency as well as the Regione Lombardia. In 2011 twenty new research projects were evaluated during four plenary sessions of the Committee. More of 50 % of the applications involved phase III trials on medicinal products, almost 40 % investigation plans on innovative medical devices and the remaining 10 % observational studies. A favourable opinion was expressed in all studies, requiring changes only on the patient information. Twenty-four applications of substantial amendments on ongoing studies were evaluated and a favourable opinion was expressed in all cases. Finally the Committee expressed a favourable opinion for the treatment with advanced, though still under investigations, techniques of two patients affected by otherwise untreatable coronary disease. CCM — Scientific Report 2011 — Ongoing research 2012 29 Library Education and Training Centro Cardiologico Monzino holds a number of on-line subscriptions to specialized journals. so to guarantee up-to-date information for medical staff and researchers. Article research is made on-line using a link connecting to the subscription list. Morever, Centro Cardiologico Monzino is member of BIBLIOSAN, the Italian library system under the supervision of the Ministry of Health, involving all IRCCS, the Istituto Superiore di Sanità, the Experimental Zooprophylactic Institutes and other healthcare institutions. It allows our staff to have access to about 5500 electronic and full-text periodicals, to RefWorks, a bibliographic management software which uses bibliography citations, to NILDE, the Network for Inter-Library Document Exchange, (allowing Centro Cardiologico Monzino to receive and send articles all over Italy), to ISI Web of Science and the Journal Citation Reports both providing data on citations and Impact Factors, to BMJ Best Practice, an innovative system for clinical decision support. The library is also member of ACNP, the National Collective Catalogue of Periodicals, an on-line catalog of printed journals which links over 2300 libraries in Italy for a total of 110.000 journals All full text publications of our medical and scientific staff are available on Centro Cardiologico Monzino web site which is updated day by day to give a complete view of the research projects and to inform the personnel of the ongoing scientific production. The Scientific Secretariat is an important help desk for researchers promoting the exchange of data among different professional areas and specialisations and, above all, between researchers of our Institute and the scientific world. Medical education is a lifelong, continuous and ongoing process throughout the professional career of healthcare providers. The university staff of the Department of Cardiovascular Sciences and the Centre of Pharmacological Research for the Study and Prevention of Cardiovascular Diseases together with the medical staff of Centro Cardiologico Monzino is engaged in a continuing education program aiming at maintaining health care at the highest level. They offer a full range of speciality and subspeciality education in the cardiovascular field. A variety of educational strategies has been carried out: formal courses, skills workshops, seminars, symposia and conferences, all addressed both to internal and external health operators. During 2011, practical and/or theoretical courses for medical staff, nurses and technicians were held at Centro Cardiologico Monzino on the following topics: • Beta blockers and heart failure • Cardiac computed tomography • Cardiopulmonary exercise testing • Carotid artery stenting • Echocardiography • Endomyocardial biopsy for electrophysiologists • Interventional cardiology • Intravascular imaging • Mapping and ablation of ventricular arrhythmias • Mitral regurgitation • Pericardial puncture and epicardial mapping • Transseptal puncture for electrophysiologists • Vascular Ecocolordoppler Besides, several seminars and scientific meetings involving both physicians and researchers were organized at Centro Cardiologico Monzino (see p. 248 for a full list). To develop the professional skills and performances of nurses, technicians (radiology and laboratory technicians, perfusionists) and physiotherapists working 30 CCM — Scientific Report 2011 — Ongoing research 2012 in the Institute, an Internal Education Program was created by the Health Professional Working Group (see p. 45). Its activity is aimed at improving health staff skills in handling emergency situations and developing the use of new technologies applied to health. It includes courses on the following topics: • Basic Life Support and Defibrillation (BLSD) • Re-training BLSD • Advanced management of cardiac emergency • ECGs for nurses (Arrhithmias, Acute Coronary Syndrome, Cardiac Pacing and Electrophysiology) • Risk prevention by patient handling • Peripheral venous catheterization • Water balance in cardiac patients • Evidence Based Practice: the future of health professionals • Prevention, assessment and treatment of skin lesions • Noninvasive ventilation Some of these courses, particularly BLSD, are required by CCM — Scientific Report 2011 — Ongoing research 2012 31 Medical Director’s Report Lorenzo CAMMELLI, MD Medical Director JCI (Joint Commission International) and IRC (International Resuscitation Council) to ensure that all personnel of the Institute is trained and updated every two years on the protocols to be used in case of cardiac arrest. In 2011 the following courses have provided a total of 2388 credit points awarded by the Ministry of Health and involved 354 people. World Heart Day The World Heart Day was created to inform people that heart disease and stroke are the world’s major causes of death. Unhealthy diet, physical inactivity and smoking are the leading causes of heart disease and stroke. To reduce the incidence of cardiovascular disease risk, prevention is fundamental. Since 2000 Centro Cardiologico Monzino has been sustaining the World Heart Federation, organizing, every year, the Monzino World Heart Day. This successful event, usually held on the last weekend of September, deals with a specific prevention topic and calls hundreds of people coming from Milano and surroundings. In 2011 the World Heart Day prevention campaign focused on workplace heart wellness. Seminars and lectures were held on cardiovascular risks on workplace, environmental stress and heart health, physical activity at work and outdoor healthy eating. A “healthy lunch” was offered to all participants. 32 CCM — Scientific Report 2011 — Ongoing research 2012 At the end of 2011, the Monzino health care clinical staff included 111 physicians, 43 medical residents, 244 registered nurses, 14 lab technicians, 6 rehabilitation technicians, 14 radiology technicians and 8 cardiology technicians (pump specialists and sonographers). In 2011 hospital admissions were 8085 (with a 2.75% decrease compared to 2010), 6841 in cardiology and 1.244 in surgery. This clinical inpatient activity produced 50.287 hospital days (34.961 in cardiology and 15.326 in surgery) with a decrease (-1.07%) compared to the previous year (50.831 in 2010). The average length of stay was 6,6 days, with an increase of 8,9% (6,06 days in 2010). The ratio between surgical admissions and total admissions (“surgical index”) was of 15.39% (16.7% in 2010). Case mix complexity, represented by the Average Relative Weight, was 1,65. The Emergency Unit treated 9.745 patients and the high rate of severe diseases led to 2054 direct admission to the clinical wards (including 145 primary PCI in the catheterization lab for acute myocardial infarction). During 2011 Centro Cardiologico Monzino further developed Transcatheter Aortic Valve Replacement (TAVR) with 123 interventions (total amount from late 2007 is 330). Furthermore, we developed percutaneous mitral valve repair, with 7 patients treated (MitraClip procedure), and artificial heart implant (2 patient had Jarvick machines). The outpatient department showed a further growth with 45.582 consultations (3.6% increase compared to 2010). CCM — Scientific Report 2011 — Ongoing research 2012 33 Acute care: mean lenght of stay Clinical Activity 2011 20 8.085 Emergency Unit (episodes of care) 9.745 Catheterizations lab patients 3.999 PCI 2.189 Electrophysiology studies and/or ablations 1.060 Cardiac surgery procedures 798 Vascular surgery procedures 616 15 Days Inpatients CYP3A4 Inhibitors/Substrates Cyclosporine, tacrolimus Macrolides (azithromycin, clarithromycin, erythromycin) Azole antifungals (itraconazole, ketoconazole) Calcium antagonists (mibefradil, diltiazem, verapamil) 45.582 Outpatients visits 10 Others Digoxin Fibrates (gemfibrozil) 5 Niacin 0 Nefazodone Protease inhibitors (amprenavir, indinavir, nelfinavir, nitronavir, saquinavir) Sildenafil Warfarin 1998 1999 2000 2001 2002 2003 2004 2005 2006 2007 2008 2009 2010 2011 CCM Acute Care: inpatients Cardiology Surgery Acute care occupancy PERIPROCEDURAL AND IN-HOSPITAL RESULTS 9000 8153 7671 7845 SUCCESS IN IMPLANTED PATIENTS: 6969 7070 6765 6890 7000 6148 PROCEDURAL 6000 5556 5000 7257 SUCCESS: 8044 8314 8085 162/163 (99,4%) 162/164 (98,8%) INTRAPROCEDURAL MORTALITY: 2/164 (1,2%) EMERGENCY SURGICAL CONVERSION: 1/164 (0,6%) Occupancy % 8000 8130 100 75 4000 3000 50 2000 Inpatients Boca 0 34 1998 1999 2000 2001 2002 2003 2004 2005 2006 2007 2008 2009 2010 2011 1000 74 64 1998 1999 2000 2001 2002 2003 2004 2005 2006 2007 2008 2009 2010 2011 CCM — Scientific Report 2011 — Ongoing research 2012 Total Cardiology Surgery CCM — Scientific Report 2011 — Ongoing research 2012 35 Casualty department (emergency) Surgical procedures (vascular) 400 10000 9331 8177 7987 8611 8701 9424 9802 9745 8836 300 7520 7510 7195 6577 Patients 5956 200 5000 100 0 0 1998 1999 2000 2001 2002 2003 2004 2005 2006 2007 2008 2009 2010 2001 2011 Surgical procedures (all) 2002 2003 2004 Vascular Surgery 2005 2006 2007 Enduvascolar total 2008 2009 2010 BOCA Surgery 2011 DX angio Interventional Cardiology 1200 2205 939 939 1166 1305 1576 1780 1927 2076 1906 1921 1991 2047 2189 813 656 600 1928 2180 2402 2337 2209 2012 2000 1820 1790 0 2001 2002 Cardiac Surgery 36 2003 2004 2005 2006 Vascular surgery CCM — Scientific Report 2011 — Ongoing research 2012 2007 2008 2009 Endovascular 2010 2011 Other surgery 1788 1998 1999 2000 2001 2002 2003 2004 2005 2006 2007 2008 2009 Cath lab total PCI Dx procedures 2022 2010 1988 2011 Altro (pfo, etc) CCM — Scientific Report 2011 — Ongoing research 2012 37 Primary PCI procedures for AMI Pace-maker and ICD 800 150 150 141 136 100 100 92 130 141 139 132 700 133 124 600 500 100 95 400 300 50 200 43 100 0 1998 1999 2000 2001 2002 2003 2004 2005 2006 2007 2008 2009 2010 0 1998 1999 2000 2001 2002 2003 2004 2005 2006 2007 2008 2009 2010 2011 2011 Acute AMI Procedures PM Electrophisiology ICD Total Out-Patient Department 2319 Encounters 2236 2129 1946 50000 2120 1915 43893 1790 39857 40000 1381 1367 1436 34016 1103 1103 30000 800 846 628 342 427 484 290 676 619 338 458 503 465 494 878 902 942 910 899 963 925 38 CCM — Scientific Report 2011 — Ongoing research 2012 28600 29621 1060 41004 41462 36120 35978 30623 25859 20000 21905 944 1036 1016 1166 1195 1998 1999 2000 2001 2002 2003 2004 2005 2006 2007 2008 Total 1093 45582 Dx ablation 1226 1176 16615 10000 2009 2010 2011 Other elph procedures 0 1998 1999 2000 2001 2002 2003 2004 2005 2006 2007 2008 2009 2010 2011 CCM — Scientific Report 2011 — Ongoing research 2012 39 Echocardiography Exercise Stress Test 10.000 25.000 20.000 7.500 15.000 5.000 10.000 2.500 5.000 0 0 1998 1999 2000 2001 2002 2003 2004 2005 2006 2007 2008 2009 2010 2011 1998 1999 2000 2001 2002 2003 2004 2005 2006 2007 2008 2009 2010 2011 2198 4090 4235 5315 5177 7006 7779 8765 8964 9266 10548 11857 12414 12756 1784 2957 3132 3251 3276 3604 4591 5128 5316 5694 5390 6300 7012 7519 6394 7011 7481 7724 8298 8020 8487 8628 8816 10565 10616 10017 10310 10875 1089 802 627 586 518 323 321 351 402 474 563 460 374 358 2006 2007 2008 Outpatient Inpatient Outpatient Holter Ecodoppler (vascular) 9.000 10.000 6.750 7.500 4.500 5.000 2.250 2.500 0 0 1998 1999 2000 2001 2002 2003 2004 2005 2006 2007 2008 1209 2856 3285 3703 3316 4108 4524 4829 4961 6355 5337 1531 1432 1304 1157 1052 981 1027 1190 1215 1248 1097 Outpatient 40 Inpatient CCM — Scientific Report 2011 — Ongoing research 2012 Inpatient 1998 1999 2000 2001 2002 6810 383 2019 2474 3156 1158 796 951 1216 1101 2010 2011 5841 6695 1108 1292 2009 2003 2004 2005 3036 4136 4030 4516 5113 4914 1542 1306 1611 1215 1288 1346 Outpatient 2009 2010 2011 6243 5193 6218 7255 1644 2038 2215 2558 Inpatient CCM — Scientific Report 2011 — Ongoing research 2012 41 Medical Directorate's Staff MEDICAL OFFICE Medical Director: Lorenzo Cammelli, MD Office Manager: Rosalba Bergami Assistant Medical Director: Ludovica Tagliabue, MD, Marta Saronio, MD Consultants: Luigi Molendini, MD, Massimo Monturano CASE-MIX & CLINICAL PATHWAYS MANAGEMENT OFFICE Administrative Staff: Francesca Ricci, Carmen Bagnardi, Manuela Pettignano, Paola Ingegneri CLINICAL PATHWAYS OFFICE Registered Nurse: Franca La Rosa, Caterina Loschiavo Consultant: Filippo Cazzulani, MD Administrative staff: Manuela Pettignano MEDICAL RECORDS OFFICE Office Manager: Elisabetta Fiore DRG & Hospital Statistics: Emanuele Martella Administrative Staff: Anna Ferragina, Luisa Passannante, Cosimo Bruno CLINICAL AUDIT & PATIENT EDUCATION OFFICE Office manager: Maria Cristina Ghidini 42 CCM — Scientific Report 2011 — Ongoing research 2012 NURSING OFFICE Head Officer: Massimo Moro Vice-Head Officer: Oriana Ferrari QUALITY & OCCUPATIONAL SAFETY Quality Manager: Fabio Tealdi Consultants: Roberta Campiglio, MD, Giovanni Morselli, MD OUTPATIENT DEPARTMENT Coordinator: Francesco Pesoli, MD Head Nurse: Laura Carparelli STERILIZATION SERVICE Head Nurse: Ornella Garganese Registered Nurses: Daniela Pozzi Quality Manager: Monica Perazzani PATIENT SAFETY & CLINICAL RISK MANAGEMENT Risk Manager: Giansaverio Friolo PHARMACY Pharmacist: Susanna Dellepiane, Laura Ricci OPERATIVE BLOCK Coordinator: Lorenzo Cammelli, MD BOP Manager: Michela Ravelli CCM — Scientific Report 2011 — Ongoing research 2012 43 Clinical Governance at Centro Cardiologico Monzino Centro Cardiologico Monzino is strongly committed to quality and safety in the treatment of cardiovascular diseases. Continuous monitoring and analysis of the provided health care are regularly performed. The implementation of innovative treatments, improvement of consolidated strategies and identification of relative weakness are addressed by multidisciplinary teams that operate with the methodology of “Strategic Process Improvement”. Beginning in the second quarter of 2008, Centro Cardiologico Monzino experienced a redesign of hospital processes, obtaining improvements in the essential clinical pathways. Innovative processes and original methods are actively discussed and implemented to improve clinical performance. The search for a more efficacious model of governance is central in the Institute’s mission, outlined by the declaration: “Centro Cardiologico Monzino aims at reaching excellence in the field of prevention, diagnosis and treatment of cardiovascular diseases, through the development of clinical-scientific research and organizational and managerial innovation, in a context characterized by a firm attention to the quality of the services provided to the patients”. In the last years more than 20 projects of management were developed in partnership with the Centro di Ricerche e Studi in Management Sanitario (Ce. Ri.S.Ma.S.). During 2011 significant improvements were developed in the areas of Clinical and Outpatient pathways and Clinical Audit and HTA and pathways, under the supervision of dr. Lorenzo Cammelli, in the areas called Cath Lab Management, under the direction of dr. Giovanni Teruzzi, and in the area of Hospital wide ECG Management System and Coronary Care Improvement, managed by dr. Giancarlo Marenzi. Quality and safety care are specifically carried out performing surveillance and control of hospital infections, pharmacological errors’ prevention, monitoring and evaluation of outcome through clinical audits, promotion of generic and specific treatment 44 CCM — Scientific Report 2011 — Ongoing research 2012 appropriateness, equity in access to healthcare, respect of regulations and deontology, professional growth, humanization and environmental comfort. In the perspective of cross-disciplinary and cooperative work, many committees operate permanently at Centro Cardiologico Monzino. They are: 1. Director’s Committee 2.Hospital Infections Committee 3. Patient Safety and Clinical Risk Management Committee 4.Drugs and Medical Devices Committee 5.Health Education Committee 6.Clinical Management Resources Committee Among the methodologies used to reach and maintain high quality standards, the adherence to principles of Clinical Governance, that provide for a strong involvement and responsibility of health operators in the clinical design processes, are particularly important. Clinical Governance at Centro Cardiologico Monzino is developed in all the components described in scientific literature: performance evaluation, quality of care, patient safety, clinical audit, patient education, evidencebased medicine and customer satisfaction. Hospital Pharmacy The Hospital Pharmacy is an essential service of the Medical Office staff. It is involved in managing supply and stocks of medicines (drugs, vaccines, and experimental drugs), dressing materials, medical devices, antiseptics and disinfectants. Hospital Infection Committee The Hospital Infection Committee works in order to continuously improve the watch and control of hospital infections. In a perspective of collaborative work, key elements are the epidemiological nurse, devoted to ward and services surveillance, and the clinical microbiologist. Patient Satisfaction During the last years, Centro Cardiologico Monzino invested large amounts of time and money to facilitate patient wellness and satisfaction. A new customer satisfaction’s system was developed to join the effective quality of health assistance and how patients perceive it. The patient satisfaction surveys (demanded by Lombardia Region to all Health Institutions, for outpatient department services and inpatient area) are performed every six months. Data are collected and analyzed with an appositely developed software and results are periodically sent to the local regulation centre (ASL) and both to Centro Cardiologico Monzino General Management and Quality Office. Clinical Audit In 1998 Centro Cardiologico Monzino started an experimental program of review focused on the most critical cardiovascular procedures, in order to obtain an improvement of clinical healthcare through its critical appraise. The Cardiovascular Surgery was the first scrutinized department. Later, Interventional Cardiology procedures were analyzed and in 2008 a clinical audit was performed in the Arrhythmology area. In 2009 the strategic project “Clinical Audit” was implemented, further increasing the analysis of Centro Cardiologico Monzino’s activities, expanding the concept of self evaluation and periodical discussion of clinical performance. Patient Education Since 2009, a comprehensive program of patient education has been developed by an interdisciplinary committee. Principal output of the program is the publication of booklets and innovative information media. In cooperation with all the health operators, the booklets are constantly increasing in number and updated, to improve patients’ information about important topics related to cardiovascular diseases and quality of life (i.e. treatments, food intake, rehabilitation, physical activities). Health Professional Working Group Patient Safety and Clinical Risk Management Patient safety program has been performed since 2005, with the creation of the Patient Safety and Risk Management Committee and the nomination of a Risk Manager figure. In these years, 11 Root Cause Analyses of problematic cases have been performed. Furthermore, regular meetings were activated to analyze the most serious events happened. In June 2007, a collaboration with other structures considered leaders in the field of safety promotion was started. In the same period, a survey to evaluate the operators’ opinions about patient safety was performed, in order to monitor the knowledge about the topic in our Institute. Modus operandi The Health Professional Working Group (nurses, health technicians and physiotherapists) meets monthly to discuss professional development of the personnel in order to develop advanced skills in the cardiovascular area and to improve the patient quality of life by reducing the impact of cardiovascular diseases and ensuring a higher and higher assistance quality. The Group also plans events, courses and seminars and works to foster the development of cardiology and cardiovascular nursing through scientific exchanges and personal contacts establishing standard of training for those who work in the cardiovascular field. Head Officer: Massimo Moro Vice-Head Officer: Oriana Ferrari Members: Pierangela Andreoletti, Gabriele Bucca, Felicia Bucci, Laura Carparelli, Mario Diomete, Ivana Favini, Luisa Fumagalli, Ornella Garganese, Maria Cristina Ghidini, Annarita Leardi, Emanuela Pagani, Rocca Punzi, Marialena Ranghetti, Fabiana Rossi, Paola Rumi, Laura Schiaroli, Giuseppe Squilla. CCM — Scientific Report 2011 — Ongoing research 2012 45 Developing Internal Education Management and continuous assistance of people with cardiovascular pathologies, prevention and rehabilitation services both inside and outside the hospital context, are specific skills of nurses, physiotherapists and technicians. Nurses, in particular, always need to follow up to date programs allowing them to effectively assist people in the best way, guarantee continuity of cares and plan and implement education services for teaching patients and their families how to self manage the illness. The Health Professional Working Group participates in the education and training of the health 46 CCM — Scientific Report 2011 — Ongoing research 2012 operators. During 2011, 10 different courses were held and administered to 354 internal operators for a total of 2388 credit points awarded by the Ministry of Health (see p. 31 for a detailed list). Besides the specific courses attended by people working in the Institute, the Group is involved in projects and events in cooperation with other institutions. In November 2011 a master in “Nursing in the Cardiovascular Area” sponsored by the Milano University, has been activated for a total of 16 participants coming from Northern Italy. CCM — Scientific Report 2011 — Ongoing research 2012 47 Cardiovascular Tissue Bank Gianluca Polvani, MD Director Co-Director and Technical/Scientific Referee: Luca Dainese, MD STAFF Technical/Organizative Referee: Anna Guarino Technician: Barbara Micheli, Francesca Prandi 48 CCM — Scientific Report 2011 — Ongoing research 2012 The activity of the Cardiovascular Tissue Bank consists in the procurement of human valves and vessels from multiorgan or cadaveric donors and in their proceeding, cryopreservation, validation for distribution and clinical employment. Tissues are usually employed in aortic ring abscess, reoperation of valvular substitution (valve degeneration), aortic ectasia, small aortic anulus, sinus Valsalve aneurysm, native vessels infections, prosthetic infections etc… The Cardiovascular Tissue Bank at Centro Cardiologico Monzino, together with the Treviso bank, is the oldest cardiovascular bank in Italy. Founded in 1992 with the name of Banca Italiana Omoinnesti (BIO), in 2005 it became the only cardiovascular bank recognized and authorized by the Regione Lombardia Health System. The bank activity, strictly connected with the CIR/CRR activity (Centro Interregionale di Riferimento/Centro Regionale di riferimento), follows both the European (Direttiva 2004/23/CE) and the Italian guidelines (19/06/2007). The bank team is available 24h-365d. Since 2005 the cardiovascular tissue bank has been certified both ISO 9001-2008 and CNT (Centro Nazionale Trapianti) for activity of “reception, proceeding, preservation and distribution of cardiovascular tissues of human origin”. It has also been registered in the European Registry of cardiovascular banks. In 2011 the bank received cardiovascular tissues from 35 multiorgan donors (Heart Beating Donor, HBD) and 6 from non heart beating (NHB) and processed 27 aortic valves, 27pulmonary valves, 17 thoracic aortas, 4 abdominal aortas with iliac arteries, 58 iliac femoral arteries, 15 safenous veins, and 1 cava vein. After preparation and anatomical, serological, microbiological evaluation, 82% of all tissues was validated and ready for distribution. During 2011, 124 tissues were distributed all over Italy. The Cardiovascular Tissue Bank is involved also in basic as well as clinical research studies. Projects concerning engineered heart valves and tissues are ongoing. Moreover, a study aimed at improving functional/mechanical/biochemical heart valve and vessel properties is being developed. Other studies about new decontamination solutions and conditions (fresh preservation) are being developed for tissue procured from organ and living donors. CCM — Scientific Report 2011 — Ongoing research 2012 49 Cardiovascular Telemedicine Gianluca Polvani, MD Director Staff: Alfreda Calligaris, MD, Amedeo Mereni, MD Head Nurse: Felicia Bucci Nurses: Francesca Bolzoni, Marina Re Secretary: Magda Ferrari The Unit is dedicated to the continuous surveillance of patients with cardiovascular diseases. This activity is carried out by a dedicated call-centre with 24h medical-nursing reference. The Unit activities are listed below: • Home-rehabilitation program after cardiac surgery procedures which ensures accurate controls especially in the first post-operative month and aims at the full reintegration of the patient in the normal daily life. This home-rehabilitation program is internationally recognized as one of the most innovative and safe program for patients with cardiac disease after cardiac surgery. Cardiologists, cardiac surgeons, physiotherapists and nurses are involved. In the call centre, medical staff with different expertise take advantage of the use of innovative devices for care and control of patients at home, providing the same safety level as the hospital • Home-rehabilitation program for heart failure patients which allows a tight control of the clinical status of the patients and provides a continuous interchange between the physician and the family doctor. This innovative management reduces the inadequate accesses to the Emergency Unit and allows a continuous update of the therapy. • Continuous electrocardiographic follow-up for arrhythmic patients with atrial and ventricular trouble (e.g. atrial fibrillation) • Home monitoring for patients waiting for cardiac surgery procedures; • Remote consulting with other institutions (for instance Europe Assistance Service) and Italian hospitals all over the world (IPOCM project). 50 CCM — Scientific Report 2011 — Ongoing research 2012 CCM — Scientific Report 2011 — Ongoing research 2012 51 Clinical Units 52 CCM — Scientific Report 2011 — Ongoing research 2012 Critical Cardiology Area Piergiuseppe AGOSTONI, MDArea Coordinator Emergency Unit 2011 Emergency Unit Alessandro SALVIONI, MD Director STAFF Deputy Directors: Fabrizio Celeste, MD, Elisabetta Doria, MD Assistants: Roberta Chiodelli, MD, Gabriella Famoso, MD, Alessandra Magini, MD, Marco Matturri, MD, Chiara Meloni, MD, Francesca Susini, MD. Fellows: Denise Brusoni, MD Head Nurse: Emanuela Pagani Nurses: Claudio Boriani, Andrea Bosis, Lorenzo Brunaccini, Ana Maria Codrenau, Margherita Corsini, Irina Alexandrina Isfan, Giuseppe Nesci, Marco Perella, Detelina Ivana Rankova, Raoul Sullcapuma Rios, Mauro Turba, Franco Vailati, Giovanni Zamboni Activities 2011. Centro Cardiologico Monzino Emergency Unit is probably the only example of emergency unit exclusively devoted to cardiac care. The Unit is equipped with nine beds provided with continuous ECG monitoring and main non invasive vital indicators (non invasive blood-pressure; oxygen saturation). Four positions are dedicated to short term observation and four to long term observation; the ninth bed is dedicated to cardio-pulmonary intensive therapy and is equipped with a DC defibrillator and a mechanical ventilator for invasive and non-invasive ventilation. The Unit is also equipped with last generation portable ultrasound devices. In the last few years the four long term observation positions have been dedicated mainly to the management of chest pain so to constitute a “Chest Pain Unit”. Patients presenting with chest discomfort not fulfilling criteria of acute coronary syndrome, are submitted to 12-18 hour observation period during which serial ECGs and measurements of markers of cardiac damage in blood are performed. In case of non diagnostic ECG and/or biomarkers, exercise testing or echo-stress (exercise stress if invaluable ECG or pharmacologic stress if unable to exercise) is carried out in order to avoid inappropriate admissions or discharges. Electric cardioversion of atrial tachyarrhytmias (more than 200 during the last year) are usually performed both for 54 CCM — Scientific Report 2011 — Ongoing research 2012 Patients % of total Patients checked Admissions Discharges Transfers to other hospitals 9745 1924 7696 125 19,7% 79,0% 1,3% Red code Yellow code Green code White code 55 814 8462 414 0,6% 8,3% 86,9% 4,2% patients admitted to the Emergency Unit and for patients hospitalized in the Acute Cardiac Care Unit. In addition, the Emergency Unit supports the telecardiology service to get ECGs of patients with heart failure, coronary artery diseases or cardiac arrhythmias. Every year about 10.000 patients suffering from cardiovascular symptoms are evaluated at this Emergency Unit. During the years a continuous increase in the access in the EU occurred and remarkably doubled in the last decade. The accuracy of these admissions is very high, with 95% of the patients presenting with cardiovascular symptoms. The most common diseases are acute coronary syndromes, heart failure, brady and tachyarrhytmias. During 2011, among all patients presenting to the Emergency Unit, 1924 patients (19,7%) were hospitalized for acute cardiac disease. In the same year, patients with “white code” (inappropriate access to the Emergency Unit for very low level of urgency) were just 4,2%. Only 125 patients (1,3%) were moved to a different hospital because of non cardiovascular disease requiring non-cardiological specialistic evaluation. During 2011 mean waiting time (from nursing triage to medical examination) for the patients classified “green- code” (patients with delayed urgency) was 49 minutes. In 2011, 1924 patients were hospitalized from the Emergency Unit; they accounted for about 24% of all admissions. Main fields of research: In 2011 the staff of the Emergency Unit and of the Acute Cardiac Care Unit evaluated the specificity and sensitivity of a new biochemical marker (copeptine) for the faster rule out of patients admitted in the EU with chest pain. The data were collected, together with other 4 Emergency Departments in Milano, and were included in the data base Rossini Trial. The Emergency Unit and the Acute Cardiac Care units were also involved in several international multicenter clinical trials on acute coronary artery disease (phase III and phase IV studies), on lipid metabolism and on diabetes in the setting of cardiovascular disease and in observational epidemiological study on atrial fibrillation: TRILOGY ACS study comparing prasugrel vs clopidogrel in patients affected by acute coronary syndrome with unstable angina/non-ST elevation myocardial infarction (UA/NSTEMI) treated with medical therapy. TRACER study evaluating the effectiveness and safety of a new inhibitor of platelet thrombin receptor (PARs) in reducing ischemic events in patients with acute coronary syndrome. CEPT Inhibitor (Roche) RO4607381: a phase III double blind randomized controlled study evaluating the effects of RO4607381 on cardiovascular risk in stable CHD patients with a documented acute coronary syndrome ALECARDIO study evaluating the efficacy of aleglitazar (receptor agonist of PPAR-alfa and PPAR-gamma) in reducing cardiovascular events in patients with type 2 diabetes mellitus and recent acute coronary syndrome. SAVOR: a multicenter phase IV trial to evaluate the effects of saxagliptin (drug of the family of incretin) on the incidence of cardiovascular death, myocardial infarction or ischemic stroke in patients with type 2 diabetes. TECOS: a randomized placebo controlled trial to evaluate cardiovascular outcomes after treatment with sitagliptin in patients with type 2 diabetes mellitus and inadequate glycemic control on mono- or dual combination oral antihyperglicemic therapy. EXSCEL: a randomized, placebo controlled clinical trial to evaluate cardiovascular outcomes after treatment with exenatide once weekly in patients with type 2 diabetes mellitus. RE-LY AF REGISTRY: risk factors, treatments and outcomes of emergency department patients with atrial fibrillation in multiple regions of the world. CCM — Scientific Report 2011 — Ongoing research 2012 55 Critical Cardiology Area Acute Cardiac Care Unit Acute Cardiac Care Unit 2011 Admissions Transfers to other units Transfers from other units Discharges Mortality rate Days of stay Alessandro SALVIONI, MD Director STAFF Deputy Directors: Fabrizio Celeste, MD, Elisabetta Doria, MD Assistants: Roberta Chiodelli, MD, Gabriella Famoso, MD, Alessandra Magini, MD, Marco Matturri, MD, Chiara Meloni, MD, Francesca Susini, MD Fellows: Denise Brusoni, MD Residents: Laura Salvini, MD, Carlo Vignati, MD Head Nurse: Mario Diomete Nurses: Katerine Barreda, Salvatore Baudanza, Filomena Briscese, Barbara Carioni, Bruna Contini, Sara Di Berardino, Jack Djoufack, Pina Granata, Ira Griffini, Adela Marcu, Veronica Meza, Mihai Mocanu, Rosa Pachas, Laura Pea, Anna Pekul, Marisa Placido, Katia Resta, Flavio Rossi 56 CCM — Scientific Report 2011 — Ongoing research 2012 979 139 40 878 1.43% 8401 Activities 2011. The activities of the Acute Cardiac Care Unit (ACCU), along with the Intensive Cardiac Care Unit, are dedicated to the diagnosis and treatment of patients admitted to the Emergency Unit for acute heart diseases. Cardiologists of the ACCU are also involved in the activity of the Emergency Unit establishing a strict cooperation with the other Units in order to reach the highest level of assistance to patients. Every year about 1000 patients are admitted to the ACCU. During 2011, this department received 51% of the patients admitted to the Emergency Unit (12% of all hospitalizations at Centro Cardiologico Monzino). In most cases (89%) the whole hospitalization until discharge was performed in the ACCU, whereas the remaining patients were moved to other Units for clinical tests and treatments. Acute coronary syndromes, congestive heart failure, severe arrhythmias (brady- and tachyarrythmias) and valvular heart diseases were the main conditions treated in the ACCU. Once admitted to the ACCU, many patients are subsequently moved to other Units according to their pathology (coronary artery bypass graft, valvular surgery including percutaneous techniques, vascular surgery). More than 100 procedures of electric cardioversion of acute and chronic atrial tachyarrhythmias were also performed during 2011. A high proportion of elderly patients admitted to the ACCU for acute cardiovascular diseases suffers also from severe medical diseases such as diabetes, chronic obstructive pulmonary disease and chronic renal failure. During 2011 ACCU was involved in 7 international phase III and IV trials aimed at assessing the efficacy and safety of new cardiovascular drugs in patients with coronary acute syndromes (2 trials), in patients with dislipydemia or type 2 diabetes and coronary disease (5 trials) and in 1 international survey study of patients affected by permanent atrial fibrillation. Publications Mega JL, Braunwald E, Mohanavelu S, Burton P, Poulter R, Misselwitz F, Hricak V, Barnathan ES, Bordes P, Witkowski A, Markov V, Oppenheimer L, Gibson CM; ATLAS ACS-TIMI 46 study group. Rivaroxaban versus placebo in patients with acute coronary syndromes (ATLAS ACS-TIMI 46): a randomised, double-blind, phase II trial. Lancet. 2009;374(9683):29-38 FUTURA/OASIS-8 Trial Group, Steg PG, Jolly SS, Mehta SR, Afzal R, Xavier D, Rupprecht HJ, López-Sendón JL, Budaj A, Diaz R, Avezum A, Widimsky P, Rao SV, Chrolavicius S, Meeks B, Joyner C, Pogue J, Yusuf S. Low-dose vs standard-dose unfractionated heparin for percutaneous coronary intervention in acute coronary syndromes treated with fondaparinux: the FUTURA/ OASIS-8 randomized trial. JAMA. 2010;304(12):1339-49 CURRENT-OASIS 7 Investigators, Mehta SR, Bassand JP, Chrolavicius S, Diaz R, Eikelboom JW, Fox KA, Granger CB, Jolly S, Joyner CD, Rupprecht HJ, Widimsky P, Afzal R, Pogue J, Yusuf S. Dose comparisons of clopidogrel and aspirin in acute coronary syndromes. N Engl J Med. 2010;363(10):930-42 Rocket AF Investigators. Rivaroxaban versus warfarin in nonvalvular atrial fibrillation. N Engl J Med 2011;365;10 P. Tricoci et al, TRACER Investigators. Thrombin-receptor antagonist vorapaxar in acute coronary syndromes. N Engl J Med 2012;366:20-33. CCM — Scientific Report 2011 — Ongoing research 2012 57 Critical Cardiology Area Intensive Cardiac Care Unit Giancarlo MARENZI, MD Director 58 CCM — Scientific Report 2011 — Ongoing research 2012 Activities 2011. The Intensive Cardiac Care Unit (ICCU) is equipped with 13 beds provided with ventilators (5 beds) and complete invasive (hemodynamic and volumetric) and non-invasive monitoring. The activity of the ICCU is mainly devoted to the treatment of patients with acute coronary syndromes (acute myocardial infarction, unstable angina) and their complications, with major acute cardiovascular events (cardiac arrest, acute pulmonary embolism, pericardial effusion, aortic dissection, life-threatening arrhythmias, conduction disturbances, acute heart failure, cardiogenic shock etc.), and, generally, with high-risk conditions. Patients with non-cardiovascular emergencies, such as acute respiratory insufficiency and acute kidney injury requiring respiratory and renal assistance, respectively, are also admitted. In 2011 the ICCU accepted about 900 patients. The ICCU staff is trained to perform noninvasive (electrocardiogram, echocardiogram, vascular echo-doppler) and invasive (cardiac catheterization, pericardiocentesis, central venous and arterial catheterization) procedures, and to support all activities in catheterization laboratories and in emergency rooms in case of cardiac arrest or need for cardiopulmonary resuscitation or emergency interventions. Both clinical and scientific activities of the Unit can be summarized as follows: 1) prevention and treatment of renal complications associated with cardiovascular diseases: acute kidney injury is frequently observed in patients admitted to this Unit because of acute cardiovascular events and hemodynamic instability, and its development is associated with relevant clinical and prognostic implications, and with increased hospital stay and costs of care. Acute kidney injury associated with acute coronary syndromes, heart failure, and contrast media toxicity is usually treated or prevented with strategies based on the application of renal replacement therapies (ultrafiltration, hemofiltration acute coronary syndromes ad other cardiovascular diseases are under investigation, in collaboration with our research and clinical laboratories. In particular, novel markers of myocardial necrosis and hemodynamic instability (high-sensitivity troponins, copeptin), myocardial reperfusion injury (cytochrome c), reduced nitric oxide synthesis (dimethylarginines), increased mortality risk (BNP, vitamin D deficiency, acute hyperglycemia), and impaired platelet activity are systematically evaluated in patients admitted to our Unit, in order to improve patients’ risk stratification and to elucidate potential mechanisms underlying acute cardiac diseases. and hemodiafiltration). In 2011 about 150 renal replacement treatments were performed. 2)pericardial effusion treatment: pericardial effusion and cardiac tamponade are common complications of cardiac surgery, electrophysiological procedures, percutaneous coronary interventions and cardiac diseases. We routinely perform pericardiocentesis under echocardiographic and radioscopic guidance as an emergency life-saving procedure. Subsequent intrapericardial treatments (antiblastic, sclerosing or anti-inflammatory therapy) are administered. In 2011 we performed about 40 pericardiocentesis 3)evaluation of novel biomarkers: novel biomarkers of Incidence of contrast-induced nephropathy (CIN) in STEMI patients with and without acute hyperglycemia, treated with primary angioplasty. eGFR = estimated glomerular filtration rate. Acute hyperglycemia No Acute hyperglycemia P=0.01 50 P<0.001 45% 38% 40 P=0.13 CIN incidence, % STAFF Senior Deputy Director: Gianfranco Lauri, MD Deputy Directors: Emilio Assanelli, MD, Marco Grazi, MD, Jeness Campodonico, MD Senior Assistants: Ivana Marana, MD Assistants: Monica De Metrio, MD, Marco Moltrasio, MD Fellows: Angelo Cabiati, MD, Mara Rubino, MD Residents: Valentina Milazzo, MD Head Nurse: Ivana Favini Nurses: Constantin Calugaru, Luisa Castellani Bencich, Roberto Cerino, Massimiliano Croce, Marisa Dolera, Tatiana Dragancea, Franca Falchi, Mercedes Maria Franco Rocha, Francesca Gaggi, Alice Giolo, Andrea Gusmaroli, Pierpaolo Iozzia, Larisa Ivanova, Pavla Kostalova, Petra Kozlova, Federica Moneta, Davide Morandi, Mariangela Alessandra Pace, Miguel Angel Pandia Palomino, Marco Riboni, Sabino Sangermano, Domenico Santoro, Veronica Barbara Sisti, Oriana Squilla, Elisabetta Volontè Secretaries: Annamaria Bellavia, Salvina Comignolo P<0.001 30 29% 27% 26% P=0.01 20 16% 10 12% 16% 11% 7% 0 n=148 n=632 n=74 n=35 n=74 n=597 n=58 n=160 n=90 n=472 All patients Diabetes No diabetes eGFR ≤ 60 eGFR > 60 mellitus mellitus ml/min/1.73m2 ml/min/1.73m2 CCM — Scientific Report 2011 — Ongoing research 2012 59 The Unit is also involved in several multicenter international trials evaluating new antithrombotic therapies for the treatment of acute coronary syndromes and for their secondary prevention. Finally, important issues of investigative interest are represented by the evaluation, diagnosis and treatment of pericardial effusions, in collaboration with Istituto Europeo di Oncologia, Milano (Cardiology Unit, Dr. Carlo Cipolla) and San Raffaele Hospital, Milano (Hematoncology and Bone Marrow Transplantation Unit, Dr. Fabio Ciceri). Publications Sisillo E, Marenzi G. N-Acetylcysteine for the prevention of acute kidney injury after cardiac surgery. J Clin Pharmacol 2011; 51(11):1603-10. Marenzi G, De Metrio M, Bartorelli A. Author’s reply to acute hyperglycemia: Is really a new risk marker for contrast-induced nephropathy in patients with acute myocardial infarction without diabetes and normal renal function? Am Heart J 2011;162:e9. 60 CCM — Scientific Report 2011 — Ongoing research 2012 Alexander JH, Lopes RD, James S, et al. for the APPRAISE-2 Investigators (G. Marenzi). Apixaban with antiplatelet therapy after acute coronary syndrome. New Engl J Med 2011;365:699-708. Oldgren J, Budaj A, Granger CB, Khder Y, Roberts J, Siegbahn A, Jan G.P. Tijssen JGP, Van de Werf F, Wallentin L, for the RE-DEEM investigators (G. Marenzi). Dabigatran vs. placebo in patients with acute coronary syndromes on dual antiplatelet therapy: a randomized, double-blind, phase II trial. Eur Heart J 2011;32:2781-2789 Cristell N, Cianflone D, Durante A, Ammirati E, Vanuzzo D, Banfi M, Calori G, Latib A, Crea F, Marenzi G, De Metrio M, Moretti L, Li H, Uren NG, Hu D, Maseri A on behalf of the FAMI Study Investigators. High-sensitivity C-reactive protein is within normal levels at the very onset of first ST-segment elevation acute myocardial infarction in 41% of cases. A multiethnic case-control study. J Am Coll Cardiol 2011;58:2654-2661 CCM — Scientific Report 2011 — Ongoing research 2012 61 Critical Cardiology Area Heart Failure, Clinical Cardiology and Cardiac Rehabilitation Unit Piergiuseppe AGOSTONI, MD Director STAFF Deputy Directors: Marina Alimento, MD, Anna Apostolo, MD, Gaia Cattadori, MD, Mauro Contini, MD, Manuela Muratori, MD, Pietro Palermo, MD, Francesco Pesoli, MD Assistants: Daniele Andreini, MD, Giovanni Berna, MD Fellows: Erika Bertella, MD, Stefania Farina, MD, Stefania Paolillo, MD, Elisa Stefanini, MD Residents: Laura Antonioli, MD, Sarah Cortinovis, MD, Erica Gondoni, MD, Giuliano Giusti, MD, Saima Mushtaq, MD, Carlo Vignati, MD Nurses: Angela Galantucci, Elena Nazzari, Maria Luisa Scapin Secretaries: Eleonora Boccato, Michela Palmieri Data Manager: Elisabetta Salvioni Activities 2011. By using advanced diagnostic tools and innovative therapeutic strategies, the Unit aims at assessing and treating heart failure, one of the most common pathologies in the western countries. The Unit provides cardiovascular rehabilitation and takes care of patients affected by heart diseases needing a “global” evaluation and drug treatment. The Unit is equipped with 36 beds and is in charge of the Cardiac Rehabilitation Gym, the Cardiopulmonary Research Laboratory, the Centre and Laboratory of Sleep Disorders, the Systemic and Pulmonary Hypertension Centre, the outpatient departments of Heart Failure, the clinical Cardiology and Cardiac Rehabilitation, the telemedicine. Piergiuseppe Agostoni is Associate Professor in Cardiology at the Milano University and Associate Professor in Critical Care and Respiratory Medicine at the University of Washington, Seattle, WA. At present, he is president of CPX International (formerly ISEIRE, International Society for Exercise Intolerance Research and Education), the Australia based Society (http://www.cpxinternational.com/) dedicated to teaching Cardiopulmonary Exercise Testing (CPET). Under the endorsement of the University of California and later of CPX International/ISEIRE, each year a 3-day CPET course is organized in different European institutions (including Centro Cardiologico Monzino) and in the last two years also in South America. Similar courses are organized in the United States, Japan and Australia. Since 1995 a 2-day CPET course, and more recently weeklong stages, have been organized by the Monzino cardiopulmonary researchers for Italian specialists with a bulk of around 1000 attendees. Moreover, Piergiuseppe Agostoni has an active role in international cooperation and specifically, through the support of the Corti Foundation (htpp://www.fondazionecorti.it/), with cardiology teaching and cardiac patients care at St Mary 62 CCM — Scientific Report 2011 — Ongoing research 2012 Lacor Hospital in Gulu (Uganda) where he spends, starting from 1978, one month per year almost every year. In the Cardiopulmonary Research Laboratory of the Centro Cardiologico Monzino, patient care and research merge in a single work so that excellence in treatment and research are connected to each other. The Cardiopulmonary Research Laboratory is the result of a total integration of the Centro Cardiologico Monzino staff and the Department of Cardiovascular Sciences staff so that it is now impossible to separate the two original components. The strength of the laboratory is the team work so that cardiologists, nurses and researchers work together to achieve their objectives. Several junior researchers before, during and after their Cardiology Fellowship Program as well as some foreign researchers participate to the activities of the Laboratory. Several grants have been offered to and by the Cardiopulmonary Research Laboratory to allow external researcher to have a training or to spend a sabbatical period of time in our laboratory. The major research topics include: a) Cardiopulmonary interactions in heart failure patients. In the last 20 years, research performed in our Unit has allowed significant advances with important implications CCM — Scientific Report 2011 — Ongoing research 2012 63 in the clinical field. Indeed, we showed that tidal volume changing during exercise predicts the exercise capacity of heart failure patients and any treatment able to improve tidal volume, e.g. ultrafiltration, increases exercise performance. b) Beta-blockers influence on exercise performance in heart failure patients. Research performed in our Unit showed that beta-blockers, which are able to improve clinical condition and prognosis of heart failure patients, do not improve maximal exercise performance but increase submaximal exercise performance. Indeed, we showed that beta-blockers, and specifically carvedilol, reduce exercise induced hyperventilation as shown by a lower VE/VCO2 slope and a higher PaCO2 during exercise. This effect is specific of non selective beta-blockers and is not shared by selective beta1-blockers. On the other side of the coin, we showed that when hyperventilation is needed, such as at high altitude, exercise performance is reduced in carvedilol treated subjects. c) Adaptation to high altitude. Several research projects have been carried out on high altitude cardiovascular adaptation in normal subjects and heart failure patients using both a high altitude model and “on-site” studies (Capanna Regina Margherita, 4600 m and Mount Everest South Base Camp, 5400 m). Particularly, we evaluated the time course and the mechanisms responsible of lung fluid movement across the alveolarcapillary membrane when reaching high altitude and adaptation in time. d) Gas exchange in heart failure. 64 CCM — Scientific Report 2011 — Ongoing research 2012 This specific topic has been heavily studied in our Unit demonstrating the presence of active mechanisms regulating the alveolar-capillary membrane permeability and the role of several drugs on it. Indeed, we showed that ACE-inhibitors improve lung diffusion, whereas aspirin and not selective beta-blockers reduce lung diffusion and AT1 blockers and selective beta1-blockers have no impact on lung diffusion. Moreover, we set up a pulmonary edema model using acute saline infusion and high altitude as such. e) Non invasive cardiac output determination during exercise. For the first time, we showed that cardiac output during exercise can be measured in heart failure patients by an inert gas rebreathing technique. This cardiac output measuring technique is now used to study, during exercise, heart failure treatment efficacy such as cardiac resynchronization therapy, mitral insufficiency correction by mitral clip and cardiac rehabilitation. By means of an international collaborative study with the University of Bern, interesting data concerning the distribution of blood flow during exercise were obtained. We also studied the role of anemia in exercise performance in chronic heart failure patients, evaluating, for each patient, the specific importance of anemia to explain functional limitation. Moreover we evaluated the effect of Ventricular Assistance Device (Jarvik) during exercise at different cardiac output settings. Finally we studied normal subjects, at present 300 of the planned 500, to measure the normal cardiac output at peak exercise in a wide population to build up and upgrade the available tables of normality which were based on old research involving a limited number of subjects due to the invasive characteristic of previously available measurement technique. f) The role of cardiopulmonary exercise testing in heart failure patients. We performed single and multicenter pathophysiological studies. We used either our database which collects data on about 1000 heart failure patients, including cardiopulmonary exercise tests and follow up, or a multicentre database, coordinated by our Unit, with more than 3500 enrolled patients. We are building a score for estimating survival in HF patients based on metabolic exercise, cardiac and kidney parameters (MECKI score). In a sub-study involving the patients with advanced HF, we are evaluating the improvement of survival in the modern era arising doubts about the actual heart transplant criteria. We also evaluated by CPET HF patient underwent to CRT showing that CRT efficacy depends on proper positioning of the LV lead over the posterolateral wall and, in the setting of unfavorable CS branches of anatomy, CRT by a surgical mini-thoracotomic approach is preferable to trans-venous lead implantation. g) The role of cardiopulmonary exercise testing in the clinical management of patients affected by pulmonary CCM — Scientific Report 2011 — Ongoing research 2012 65 arterial hypertension. Patients affected by pulmonary arterial hypertension (PAH) show a reduced exercise tolerance with early occurrence of dyspnea and fatigue. The origin of functional capacity limitation is multifactorial and several mechanisms have been proposed, including right heart failure, which leads to a limited increase in cardiac output during exercise, and hyperventilation with a reduced perfusion of properly ventilated alveoli. In addition, abnormalities in arterial blood gases are observed, with the occurrence of hypoxemia and hypocapnia, related to an abnormal ventilation/perfusion match, gas diffusion abnormalities, low mixed venous oxygen saturation and to the development of intra- and extra-pulmonary right-to-left shunts. At present, the 6-minute walking test is the most used method to assess exercise tolerance in PAH; it is also useful to monitor the response to therapy and provides prognostic information. However, the assessment of functional capacity by cardiopulmonary exercise test (CPET) seems to be more complete, because CPET allows for discrimination between the metabolic, cardiovascular and pulmonary components of exercise limitation. Moreover, CPET estimates the severity of disease and assesses patient prognosis and response to therapy. In PAH, a typical CPET-response is observed, characterized by a severe reduction in peak VO2, work rate, O2 pulse and anaerobic threshold and by a marked increase in VE/VCO2 slope and in the dead space to tidal volume ratio. However, the use of CPET should be limited to experienced centers. This review will focus on resting lung function and exercise tolerance tests, showing that CPET can provide the physiological explanation of functional limitation in PAH. h) The role of plasma SPB and RAGE as markers of lung injury. We studied plasma SPB and RAGE during mechanical ventilation in patients undergoing major vascular surgery and in the plasma during cardiopulmonary bypass. We 66 CCM — Scientific Report 2011 — Ongoing research 2012 identified a different kinetics between SPB and RAGE during lung acute damage. Indeed SPB seems to be more strictly related to the lung than RAGE. This allow us to suggest a role of SPB as a lung damage marker. Other research trials on exercise physiology in heart failure, heart failure treatment, heart failure rehabilitation and evaluation of heart failure prognosis, have been done or are ongoing. Within the Unit, the Cardiac Rehabilitation (Rehab) is a program designed to help improving the patient overall health. The program promotes life-style changes and medical management to: • prevent the occurrence and/or progression of cardiovascular diseases • reduce the risk of a heart attack or stroke • reduce the need for future surgery • enhance the quality of life by reducing symptoms An exercise physiologist or a qualified nurse helps patients to attain their personal goals. Cardiac Rehab programs is addressed to patients with: • coronary artery bypass graft (CABG) surgery • heart attack (myocardial infarction) • heart failure Soon after the discharge from the hospital, the patient can enter the outpatient Cardiac Rehab program. All sessions are medically supervised and directed by nationally certified rehabilitation specialists and nurses. State-of-the-art monitoring equipment and a variety of exercise equipments are available. G, Andreini D, Tondo C, Agostoni PG. Long-term effectiveness of cardiac resynchronization therapy in heart failure patients with unfavorable cardiac veins anatomy comparison of surgical versus hemodynamic procedure. J Am Coll Cardiol. 2011;58(5):483-490 Karsten M, Contini M, Cefalù C, Cattadori G, Palermo P, Apostolo A, Bussotti M, Magrì D, Salvioni E, Farina S, Sciomer S, Catai AM, Agostoni P. Effects of carvedilol on oxygen uptake and heart rate kinetics in patients with chronic heart failure at simulated altitude. Eur J Cardiovasc Prev Rehabil. 2011 (Epub ahead of print) Agostoni P, Swenson ER, Bussotti M, Revera M, Meriggi P, Faini A, Lombardi C, Bilo G, Giuliano A, Bonacina D, Modesti PA, Mancia G, Parati G; HIGHCARE Investigators. High-altitude exposure of three weeks duration increases lung diffusing capacity in humans. J Appl Physiol. 2011;110(6):1564-1571 Agostoni P, Banfi C, Brioschi M, Magrì D, Sciomer S, Berna G, Brambillasca C, Marenzi G, Sisillo E. Surfactant protein B and RAGE increases in the plasma during cardiopulmonary bypass: a pilot study. Eur Respir J. 2011;37(4):841-847 Publications Cattadori G, Schmid JP, Brugger N, Gondoni E, Palermo P, Agostoni P. Hemodynamic effects of exercise training in heart failure. J Card Fail. 2011;17(11):916-922 Giraldi F, Cattadori G, Roberto M, Carbucicchio C, Pepi M, Ballerini G, Alamanni F, Della Bella P, Pontone CCM — Scientific Report 2011 — Ongoing research 2012 67 Interventional Cardiology Area Antonio BARTORELLI, MD Area Coordinator Interventional Cardiology Units Antonio BARTORELLI, MD Director of Unit 1 Piero MONTORSI, MD Director of Unit 2 Alessandro LUALDI, MD Director of Unit 3 Franco FABBIOCCHI, MD Director of Unit 4 STAFF Senior Deputy Directors: Luca Grancini, MD, Paolo Ravagnani, MD Deputy Directors: Stefano Galli, MD, Daniela Trabattoni, MD Assistants: Giuseppe Calligaris, MD, Stefano De Martini, MD, Giovanni Teruzzi, MD Residents: Maria Antonietta Dessanai, MD, Pamela Gatto, MD, Marco Valerio Morpurgo, MD, Paolo Olivares, MD, Chiara Stefania Pandini, MD, Francesca Pizzamiglio, MD Fellows: Cristina Ferrari, MD, Anna Garlaschè, MD, Massimo Mapelli, MD, Ilaria Previtali, MD Head Nurse: Gabriele Bucca Nurses: Mariangela Alberti, Gabriella Battaini, Francesca Bonfiglio, Daniele Buono, Ivan Consoli, Fernanda Giancola, Rossella Paloschi, Gabriella Panetta, Gaetano Seletti, Enrico Speranza Chief Technician: Giuseppe Squilla Technicians: Vania Battaglini, Chiara De Pasquale, Vincenzo Lo Mascolo, Flavio Mu, Stefania Pergolizzi Secretaries: Mariagrazia Cortesi, Fernando Di Marino 68 CCM — Scientific Report 2011 — Ongoing research 2012 Activities 2011. Interventional cardiology is a modern branch of medicine with a very high technology content, which deals with the non-surgical management of cardiovascular diseases. The role of invasive cardiology has rapidly grown from a predominantly diagnostic activity to a full range of therapeutic interventions as alternatives to traditional surgical and medical treatments. The cardiac catheterization laboratories of Centro Cardiologico Monzino are equipped with the most advanced and innovative tools to offer a full range of state-of-the-art diagnostic and therapeutic procedures. Together with traditional angiography, additional diagnostic modalities such as intravascular ultrasound and virtual histology, optical coherence tomography, flowwire and quantitative angiography allow a more precise and accurate evaluation of lesion to be treated and postprocedural results. In 2010, Centro Cardiologico Monzino continued to be at the forefront of elective coronary artery disease treatment using constantly updated coronary angioplasty techniques and state-of-the-art drug-eluting stents. Patients with acute coronary syndromes were also treated using coronary angioplasty and stenting and the latest technology for protecting the coronary microcirculation, particularly in acute myocardial infarction. This patient subset can receive prompt treatment by a skilled team of interventional cardiologists available on a 24/24-hour 7/7day basis. Moreover, cardiac support devices (intra-aortic balloon pump, percutaneous cardiopulmonary support and Impella device) are available and were used to support patients with reduced left ventricular function. We also offered angioplasty and stenting in the arteries of the leg and the kidneys, the carotid arteries, and the abdominal vessels, such as the aorta and the iliacs. Interventional cardiologists also used their extensive expertise in the successfully treatment of structural heart disease using innovative therapeutic modalities such as alcohol septal ablation for hypertrophic obstructive cardiomyopathy, atrial septal defect and patent foramen ovale closure, and left atrial appendage obliteration for prevention of cardiogenic embolization in atrial fibrillation patients. In 2008, in collaboration with the Cardiac Surgery Unit, we started a minimally invasive procedure for the treatment of high-risk symptomatic patients with severe aortic stenosis using the Edwards SAPIEN transcatheter heart valve. Among preventive strategies in high-risk patients, a particular attention has been devoted to contrast nephropathy using very effective prophylactic treatments such as continuous veno-venous hemofiltration (CVVH) and novel investigational devices. Other critical collaborations continued for prevention, diagnosis and treatment of patients with cardiovascular disorders and for research purposes with the Cardiovascular Imaging Area (MDCT, 3D-echo, TEE), the Intensive Cardiac Care Unit, the Laboratory of Biology and Biochemistry of Atherothrombosis and the Laboratory of Gene Therapy. In addition to their clinical activity, many members of our Units have university and institutional teaching CCM — Scientific Report 2011 — Ongoing research 2012 69 Electrophysiology Area Claudio TONDO, MD, Ph.D Area Coordinator Electrophysiology Unit Claudio TONDO, MD, Ph.D Director Corrado CARBUCICCHIO, MD, Ph.D Director of Ventricular Intensive Unit responsibilities involving mainly student and fellow training, and are engaged in Continuing Medical Education (CME) programs. Publications Silber S, Windecker S, Vranckx P, Serruys PW; RESOLUTE All Comers investigators. Unrestricted randomised use of two new generation drug-eluting coronary stents: 2-year patient-related versus stentrelated outcomes from the RESOLUTE All Comers trial. Lancet. 2011; 377(9773):1241-7 Serruys PW, Silber S, Garg S, van Geuns RJ, Richardt G, Buszman PE, Kelbaek H, van Boven AJ, Hofma SH, Linke A, Klauss V, Wijns W, Macaya C, Garot P, DiMario C, Manoharan G, Kornowski R, Ischinger T, Bartorelli A, Ronden J, Bressers M, Gobbens P, Negoita M, van Leeuwen F, Windecker S. Comparison of zotarolimuseluting and everolimus-eluting coronary stents. N Engl J Med. 2010; 363(2):136-46 70 CCM — Scientific Report 2011 — Ongoing research 2012 Marenzi G, Assanelli E, Campodonico J, De Metrio M, Lauri G, Marana I, Moltrasio M, Rubino M, Veglia F, Montorsi P, Bartorelli AL. Acute kidney injury in ST-segment elevation acute myocardial infarction complicated by cardiogenic shock at admission. Crit Care Med. 2010; 38(2):438-44. Pontone G, Andreini D, Bartorelli AL, Cortinovis S, Mushtaq S, Bertella E, Annoni A, Formenti A, Nobili E, Trabattoni D, Montorsi P, Ballerini G, Agostoni P, Pepi M. Diagnostic accuracy of coronary computed tomography angiography: a comparison between prospective and retrospective electrocardiogram triggering. J Am Coll Cardiol. 2009; 54(4):346-55. Marenzi G, Assanelli E, Campodonico J, Lauri G, Marana I, De Metrio M, Moltrasio M, Grazi M, Rubino M, Veglia F, Fabbiocchi F, Bartorelli AL. Contrast volume during primary percutaneous coronary intervention and subsequent contrast-induced nephropathy and mortality. Ann Intern Med. 2009; 150(3):170-7. STAFF Senior Deputy Director: Stefania Riva, MD Deputy Directors: Antonio Dello Russo, MD, Ph.D, Gaetano Fassini, MD Senior Assistant: Michela Casella, MD, Ph.D Assistants: Massimo Moltrasio, MD, Fabrizio Tundo, MD, Ph.D Fellows: Benedetta Majocchi, MD, Martina Zucchetti, MD, Vittoria Marino, MD Nurses: Luana Barbieri, Rosario Cervellione, Pasquale De Iuliis, Roberta Fasana, Mario La Notte, Claudia Perlotti, Maria Lena Ranghetti, Romina Ranzato, Alberto Somenzi, Michela Vendramin Secretaries: Viviana Biagioli, Tiziana Peroncini Activities 2011. The clinical activity of the Electrophysiology Area deals with electrophysiological procedures and cardiac pacing. Electrophysiological procedure. Almost every type of arrhythmia is managed in the Electrophysiology Area: supraventricular paroxysmal tachycardia, WolffParkinson-White syndrome, atrial tachycardia, atrial flutter, atrial fibrillation, ventricular tachycardia and ventricular premature beats. Treatment consists mostly in radiofrequency catheter ablation of the arrhythmia guided by conventional mapping or, more often, after 3D reconstruction and substrate mapping. The efforts of the Electrophysiology Area mostly converge on ablation of atrial fibrillation and ventricular tachycardia. Atrial fibrillation is the most common significant cardiac arrhythmia, responsible for approximately one-third of all hospital admissions of patients suffering from cardiac rhythm disturbances. It is responsible for an increased risk of stroke, heart failure and all-cause mortality. The vast improvement over the last decade in the long term efficacy of catheter ablation, compared to pharmacological treatment, supports the use of ablation in the early management of patients suffering from atrial fibrillation. In the Electrophysiology Area catheter ablation is currently performed for paroxysmal and persistent atrial fibrillation (up to 300 per year). The procedure is usually guided by 3D electroanatomical mapping systems (Carto 3/NavX) integrated by a previously acquired CT or MRI image of the left atrium and/or intracardiac echocardiography (CartoSound technology). In the setting of atrial fibrillation, the Electrophyisology Area is also equipped to perform transcatheter closure of the left atrial appendage in order to reduce the cardioembolic risk in those patients with persistent/ permanent atrial fibrillation who are not candidates for warfarin therapy. CCM — Scientific Report 2011 — Ongoing research 2012 71 Ventricular Tachycardia. Until recently, antiarrhythmic drugs were the preferred treatment for most patients with recurrent ventricular tachycardia, whatever the underlying heart disease. However, the risk of sudden cardiac death and recurrences remains high despite drug therapy; alternative treatment options include surgical ablation, implantation of a cardioverter-defibrillator (ICD), and catheter ablation. Although ICDs prolong survival, they do not prevent ventricular tachycardia recurrences, thus being a merely palliative treatment. Catheter ablation, on the contrary, is a potentially curative approach, preventing ventricular tachycardia recurrences in more than 70% of patients. In the Electrophysiology Area catheter ablation of ventricular tachycardia is often performed in the setting of dilated cardiomyopathy, ischaemic cardiopathy, arrhythmogenic right ventricular cardiomyopathy, or in the context of an apparently normal heart, as it is often the case with right and left ventricular outflow tract tachycardia. Ablation is usually guided by 3D electroanatomical mapping systems, including noncontact systems. Moreover, the Electrophysiology Area includes a new and unique service focused on critical ventricular arrhythmias, called Ventricular Intensive Care (VIC). It strives for a “global” treatment of patients with ventricular arrhythmias responsible for critical impairment of clinical conditions and/or for multiple ICD interventions. The VIC unit aims at improving quality of life and optimizing antiarrhythmic therapies by integrating acute and long-term care provided by the same team of operators. The Electrophyisology Area is also equipped to perform endomyocardial biopsies (EMB) to improve diagnostic accuracy and prognostic correlations in the setting of cardiomyopathy, arrhythmogenic right ventricular dysplasia, myocarditis, cardiac tumors, arrhythmia, etc. 72 CCM — Scientific Report 2011 — Ongoing research 2012 The right internal jugular vein and the femoral vein are the most common percutaneous access sites for right ventricular EMB, which is usually performed safely under fluoroscopic and intracardiac echo guidance. Histological samples are also examined for genetic mutations and for amplification of viral genomes. In addition to its clinical uses, EMB may be a precious instrument to better understand the cellular and molecular pathophysiology of cardiovascular disease. Cardiac pacing. The Electrophysiology Area performs implantation and replacement of permanent pacemakers, including both single-chamber and (more often) dual-chamber devices. Each year approximately 200 implantable cardioverter-defibrillators (ICD) and/or biventricular pacemakers (for cardiac resynchronization therapy: CRT) are implanted, for the prevention of sudden cardiac death and for improvement of heart failure respectively, often in patients with severe left ventricular dysfunction and/or malignant ventricular arrhythmias. Over the last years, the technique of catheter lead extraction with the use of Locking Stylets, Telescoping Synthetic Sheaths, Electrosurgical Dissection and Laser Extraction has been implemented to answer the increased demand generated by lead damage or device infection. Publications Santangeli P, Dello Russo A, Pieroni M, Casella M, Di Biase L, Burkhardt JD, Sanchez J, Lakkireddy D, Carbucicchio C, Zucchetti M, Pelargonio G, Themistoclakis S, Camporeale A, Rossillo A, Beheiry S, Hongo R, Bellocci F, Tondo C, Natale A. Fragmented and delayed electrograms within fibrofatty scar predict arrhythmic events in arrhythmogenic right ventricular cardiomyopathy: Results from a prospective risk stratification study. Heart Rhythm. 2012 (Epub ahead of print) Santangeli P, Pieroni M, Dello Russo A, Casella M, Pelargonio G, Di Biase L, Macchione A, Burkhardt JD, Bellocci F, Santarelli P, Tondo C, Natale A. Correlation between Signal-Averaged Electrocardiogram and the Histologic Evaluation of the Myocardial Substrate in Right Ventricular Outflow Tract Arrhythmias. Circ Arrhythm Electrophysiol. 2012 (Epub ahead of print) Dello Russo A, Casella M, Pieroni M, Pelargonio G, Bartoletti S, Santangeli P, Zucchetti M, Innocenti E, Di Biase L, Carbucicchio C, Bellocci F, Fiorentini C, Natale A, Tondo C. Drug-Refractory Ventricular Tachycardias Following Myocarditis: Endocardial and Epicardial Radiofrequency Catheter Ablation. Circ Arrhythm Electrophysiol. 2012 (Epub ahead of print) Casella M, Dello Russo A, Pelargonio G, Bongiorni MG, Del Greco M, Piacenti M, Andreassi MG, Santangeli P, Bartoletti S, Moltrasio M, Fassini G, Marini M, Di Cori A, Di Biase L, Fiorentini C, Zecchi P, Natale A, Picano E, Tondo C. Rationale and design of the NO-PARTY trial: near-zero fluoroscopic exposure during catheter ablation of supraventricular arrhythmias in young patients. Cardiol Young. 2012;3:1-8. Dukkipati SR, Neuzil P, Kautzner J, Petru J, Wichterle D, Skoda J, Cihak R, Peichl P, Dello Russo A, Pelargonio G, Tondo C, Natale A, Reddy VY. The durability of pulmonary vein isolation using the visually guided laser balloon catheter: multicenter results of pulmonary vein remapping studies. Heart Rhythm. 2012 (Epub ahead of print) CCM — Scientific Report 2011 — Ongoing research 2012 73 Cardiovascular Surgery Area Francesco ALAMANNI, MD Area Coordinator Cardiac Surgery Unit 1 Cardiac Surgery Unit 2 Francesco ALAMANNI, MD Director Gianluca POLVANI, MD Director STAFF Deputy Directors: Moreno Naliato, MD, Alessandro Parolari, MD, Ph.D, Giulio Pompilio, MD, Ph.D, Maurizio Roberto, MD, Ph.D, Marco Zanobini, MD, Ph.D Senior Assistants: Francesco Grillo, MD Senior Deputy Directors: Marco Agrifoglio, MD Assistant: Samer Kassem, MD Fellow: Eleonora Penza, MD Residents: Francesco Arlati, MD, Laura Cavallotti, MD, Andrea Daprati, MD, Sara Filippini, MD, Tommaso Generali, MD, Marco Gennari, MD, Daniela Manzone, MD, Elisa Merati, MD, Gabriele Tamagnini, MD, Giulio Tessitore, MD Head Nurses: Annarita Leardi, Rocca Punzi Referent Nurses: Anna Sudati, Sara Fronterrè Nurses: Brunella Biava, Evson Capuno, Andrea Dimastrogiovanni, Francesca Fugazza, Sonia Huaman, Alin Pavel Huci, Jirina Kopecna, Ana Liliana Lasteros, Giuseppe Leontino, Monica Marino, Federica Marson, Saveria Mennuti, Tiziana Nella, Lucia Palladino, Marco Racioppo, Tommaso Sambito, Sara Sesto, Petra Skarcova, Richard Sucapuca, Alexandra Vicari, Ermes Visigalli, Operating Room Head Nurse: Maria Luisa Fumagalli Operating Room Nurses: Barbara Brizio, Maria Teresa Gallo, Rejab Jihed, Anna Ligorio, Gabriela Makrovska, Emanuela Mancino, Cristiano Moro, Brigitta Nobrega, Daniela Pedrini, Stefania Pellati, Ilaria Poppa, Simona Ravani, Chiara Rosselli, Sabrina Salerno, Jana Smerekovska, Cristina Spadotto Secretaries: Daniela Corti, Nadia Vaccari 74 CCM — Scientific Report 2011 — Ongoing research 2012 Cardiac Surgery Unit 1 Cardiac Surgery Unit 2 CCM — Scientific Report 2011 — Ongoing research 2012 75 Cardiovascular Surgery Area Activities 2011. Clinical activities involved all fields of adult cardiac surgery; in 2011 in-hospital mortality was 2,96% (coronary surgery 0%, valve surgery 2.4%, combined valve and coronary surgery 7,1%). In 2011 we performed 777 surgical interventions with a prevalence of valvular repair-replacement; there was a slight decrease in coronary surgery due to the increasing number of percutaneous treatment of this disease. Valve surgery of the adult patient very often involves aortic and/or mitral valve, with or without associated coronary revascularization procedures. Mitral valve surgery. We performed 139 procedures with an increase of very complex repairs; also, we have implemented our techniques expanding the concept of “respect vs resect”; this means that we have attempted to perform more physiologic repair procedures, trying to avoid extensive removals of mitral valve native tissue in order to preserve (“respect”) as much as possible the native anatomy of the mitral valve though warranting an optimal repair procedure. During this year a program for “Transcatheter Mitral Valve Repair” (MitraClip), in addition to the aortic valve transcatheter treatment program, has been developed and a growing number of high risk surgical patients has been treated focusing on clinical results and physiopathology of MitraClip effects on heart valves. This has been done with the cooperation of the Interventional Cardiology Units. During this year we have increased the numbers of mitral valve repairs performed by using a minimally invasive surgical approach. In addition, in cooperation with the Echocardiography Unit we have continued pre- and intraoperative studies of anatomy and mechanisms of regurgitation (with 3D-transthoracic realtime echocardiography we are able to plan the repair technique). 76 CCM — Scientific Report 2011 — Ongoing research 2012 Since mitral valve disease is frequently associated with tricuspid valve involvement, and since an untreated tricuspid valve disease at the time of mitral valve surgery may adversely affect the follow-up results, during the last year we became more aggressive in detecting and treating this disease, according to recent clinical evidence. We were also very active in studying mitral valve disease, focusing on the biological pathways activated in the course of the disease and possibly involved in the etiology of mitral valve regurgitation. In addition, together with the Echocardiography Unit and the Bioengineering Department of Politecnico of Milano, we studied mathematical and simulation models of mitral valve disease and other common techniques of repair. More recently, always together with the Echocardiography Unit and the Bioengineering Department of Politecnico of Milano and Bologna, we have focused our attention on the impact of the mitral valve on the function of the aortic valve. Concerning aortic valve surgery, during 2011 we performed 240 aortic valve replacements, with an increasing percentage of procedures done by using a minimally invasive approach; 123 of these replacements were performed with transcatheter techniques; in 20 patients we also performed aortic valve repair with anatomic reconstruction. With the advent of transcatheter techniques, aortic valve replacement can now be considered in patients who were previously off-limits for conventional open-chest surgery. This was possible thanks to the cooperation with the Anaesthesiology, Vascular Surgery, Radiology, Angiography and Echocardiography Units for preoperative assessment and intraoperative procedures. Thus we have further expanded our experience in transcatheter aortic valve replacements, with about 328 cases performed up to now with this technique. The biology of aortic valve degeneration is also a hot topic of our research: we have studied the possible protective effects of statin pre-treatment on the outcomes and on the disease progression of patients with aortic valve stenosis, showing that, when the degree of stenosis is advanced, statins may not be an effective preventive measure. We have started a program of sutureless aortic valve implantation which is clinically positioned in a midway between TAVI and conventional AVR. Using these valves it is possible to replace aortic valves by minimally invasive access and to reduce ECC time in complex procedures thus reducing trauma in the aged risk patients not candidate to TAVI . Coronary bypass surgery represented slightly less than 30% of our activity. Despite the decreasing clinical conditions and the increasing age of patients, our inhospital mortality (usually considered the indicator of care quality in a cardiac surgery program) was very low. During the last year we have been very active in multi-arterial grafting, especially in younger patients, we have continued clinical assessment of off-pump coronary bypass procedures and started exploring the potential of hybrid (surgical revascularization associated with coronary stenting) revascularization techniques. We have also recruited patients for studies on cardiovascular prevention and the role of conventional and unconventional risk factors. In addition, in cooperation CCM — Scientific Report 2011 — Ongoing research 2012 77 with the Radiology Unit, we are concluding a follow-up study involving 330 patients, previously submitted to isolated coronary bypass surgery, in order to document patency of coronary bypasses using a 64-rows CT scan 18 months after surgery and to investigate the possible predictors of bypass occlusion. The surgery of cardiac arrhythmias had an important implementation during the last year; thanks to the cooperation with the Electrophysiology Unit we started to treat surgically (via mini-incisions) patients affected by atrial fibrillation and unresponsive to conventional therapies and have recently updated the clinical protocol extending the treatment of concomitant AF in patient in whom a surgical approach to mitral valve is not planned (i.e. aortic valve and coronary revascularization) and the entire procedure is performed with the closed left atrium. We also started the isolated treatment of ventricular tachycardia due to ischemic disease, dilatative cardiomyopathy or ventricular tumour unresponsive to EPS treatments. For the first time ever, we treated 19 patients with VT. Our data collection and results are continuously monitored by a public clinical Audit accredited by the most important European agency in this field, ECTSIA (European Cardiovascular & Thoracic Surgery Institute of Accreditation). Research areas: • Genomics of coronary artery, valve and aortic disease. • Perioperative proteomic profiles of patients undergoing coronary bypass, valve and aortic procedures. • Proteomics of non-rheumatic calcific aortic stenosis, mitral valve prolapses, and aortic aneurysms. • Coagulation, inflammation and oxidative stress 78 CCM — Scientific Report 2011 — Ongoing research 2012 activation during and after coronary bypass, valve and aortic procedures. • Predictors of patency of coronary bypass grafts and of late outcome in patients undergoing coronary bypass surgery. • Biology of non-rheumatic, calcific aortic stenosis and mitral valve prolapse. • Evaluation of algorithms predicting the occurrence of perioperative acute kidney injury after adult cardiac surgery • Application of advanced statistical models to cardiac surgery. • Systematic review of the role of statins in the prevention of major complications and disease progression in non-rheumatic, calcific aortic stenosis. • Minimally invasive cardiac surgery for valve repair. • Alternative therapies for cardiac arrhythmias (atrial fibrillation, ventricular tachycardia) not responsive to conventional therapies: role of surgery. • Role of intraoperative electro-anatomic mapping (CARTO) during surgical ablations for refractory ventricular tachycardia. • Mathematical and simulation models of mitral valve disease (assessed by 3D-echocardiography) and of the most common techniques of repair. • Regenerative medicine for ischemic heart disease. • Transcatheter aortic valve implantation in calcific aortic stenosis: predictors of outcome and choice of techniques. • Clinical follow up of patients submitted to surgical treatment of concomitant or lone AF via implantable loop recorders or EPS • MitraClip in high risk patients: evaluation of cardiac performance before and after implantation, effects of the device on mitral flow and dynamics. • Sutureless aortic prosthesis: definition of anatomical pre-implant variables, impact of the device on mitral-aortic coupling • Impact of mitral valve reconstruction on the aortic valve, left and right ventricle. Publications Parolari A, Pesce LL, Pacini D, Mazzanti V, Salis S, Sciacovelli C, Rossi F, Alamanni F. Monzino Research Group on Cardiac Surgery Outcomes. Risk factors for perioperative acute kidney injury after adult cardiac surgery: role of perioperative management. Ann Thorac Surg. 2012;93(2):584-591 Cheema FH, Polvani G, Argenziano M, Pesce M. Combining stem cells and tissue engineering in cardiovascular repair -- a step forward to derivation of novel implants with enhanced function and self-renewal characteristics. Recent Pat Cardiovasc Drug Discov. 2012;7(1):10-20 Pompilio G, Filippini S, Agrifoglio M, Merati E, Lauri G, Salis S, Alamanni F, Parolari A. Determinants of pericardial drainage for cardiac tamponade following cardiac surgery. Eur J Cardiothorac Surg. 2011;39(5):e107-113 Parolari A, Tremoli E, Cavallotti L, Trezzi M, Kassem S, Loardi C, Veglia F, Ferrari G, Pacini D, Alamanni F. Do statins improve outcomes and delay the progression of non-rheumatic calcific aortic stenosis? Heart 2011;97(7):523-529 Loardi C, Alamanni F, Trezzi M, Kassem S, Cavallotti L, Tremoli E, Pacini D, Parolari A. Biology of mitral valve prolapse: the harvest is big, but the workers are few. Int J Cardiol. 2011;151(2):129-135 CCM — Scientific Report 2011 — Ongoing research 2012 79 Cardiovascular Surgery Area Cardiovascular Surgery Area Extracorporeal Circulation Service Vascular Ultrasound Service STAFF Coordinator: Marco Agrifoglio, MD, Ph.D Assistants: Luca Dainese, MD, Francesco Grillo, MD, Moreno Naliato, MD, Maurizio Roberto, MD, Claudio Saccu, MD, Stefano Zoli, MD Certified Clinical Perfusionists (CCP): Marcello Fonga, Davide Pedroletti, Gianluca Riva, Vanessa Villani STAFF Chief Perfusionist: Fabiana Rossi Certified Clinical Perfusionists (CCP): Antonella Bertera, Angelica Capozzoli, Rita Fabrizi, Marcello Fonga, Davide Pedroletti, Gianluca Riva The Extracorporeal Circulation (ECC) Service was established in 1982 with the start of cardiac surgery. With the help of specific devices, the ECC service supports the vital functions of patients undergoing cardiac surgery or interventional cardiology procedures and it is involved in all situations where patients urgently need a cardiovascular support. Since 1982, about 18.328 ECC procedures have been performed. Nowadays four operating rooms are available with a team of six technicians. The indication for use of ECC involves both cardiac and vascular surgery. Today ECC is also used as a support during cardiovascular interventional cardiology procedures and as assistance in patients with hemodynamic compromise. In 2011, 628 extracorporeal circulation procedures were performed, 4 cardiopulmonary supports, and over 200 stand-by or complex vascular interventional procedures 80 CCM — Scientific Report 2011 — Ongoing research 2012 and cardiosurgery. A teaching course for perfusionists has been available since 1988 and in 2001 it became a first level degree for cardiovascular pathophysiology. The Perfusion Education Program at Centro Cardiologico Monzino was accredited by EBCP (European Board of Cardiovascular Perfusion) in 2004. The ECC service is certified ISO 9001:2008 The Vascular Ultrasound Service was created at Centro Cardiologico Monzino in 1991 and it provides a noninvasive assessment of suspected vascular pathological conditions. The vascular scan evaluations are carried out both by cardiac and vascular surgeons with the most sophisticated ultrasound equipments available. In 2011, 9813 procedures were performed (8434 in 2010) and a number of technicians, highly trained and experienced in vascular imaging techniques, was included in the staff. Ultrasound interrogations allow to predict a wide range of diseases and conditions. Research activity • preoperative non-invasive assessment of radial artery for coronary artery bypass grafting • preoperative non-invasive assessment of carotid artery for coronary artery bypass grafting • preoperative non-invasive assessment of superficial arterial beds Educational activity. The students attending the Cardiac Surgery Postgraduate School of the University of Milano are first trained and subsequently employed in the service. To improve education of both technologists and physicians, a postgraduate course in Vascular Ultrasound is organized every year at Centro Cardiologico Monzino CCM — Scientific Report 2011 — Ongoing research 2012 81 Cardiovascular Surgery Area Vascular and Endovascular Surgery Unit Rita SPIRITO, MD Director Vascular and Endovascular Surgery Unit 2011 Surgical procedures Endovascular procedures STAFF Deputy Directors: Luca Dainese, MD, Melissa Fusari, MD, Piero Trabattoni, MD Assistants: Claudio Saccu, MD, Stefano Zoli, MD Cardiovascular Ambulatory: Amedeo Mereni, MD Head Nurse: AnnaRita Leardi Co-Head Nurse: Anna Sudati Secretaries: Nadia Vaccari, Daniela Corti Activities 2011. The Unit provides diagnosis and treatment for a wide variety of circulatory diseases such as aneurysms of the thoracic aorta and/or the abdominal aortic and its branches, extracranial cerebrovascular disease, carotid artery disease, peripheral vascular surgery of the upper and lower extremities including arterial occlusive diseases and vein disorders (varicose veins or chronic venous insufficiency). The Unit performs surgical and/ or minimally invasive endovascular techniques including: balloon angioplasty and/or stenting, aortic and peripheral vascular endovascular stent/graft placement and other adjuncts for vascular reconstruction. During 2011, 514 patients with vascular pathologies were treated. A new multifunctional operating room combining endovascular, cardiac catheterization, cardiac, surgical and radiological capabilities was opened in October 2008, allowing a team composed by vascular, cardiac surgeons and anaesthetists to perform transcatheter aortic valve implants (transfemoral or transapical approach). Nowadays the room allows, with the maximum flexibility, the treatment of patients with the most complex cardiac and vascular conditions. More than 8000 ultrasound tests were performed during the last year with the most advanced diagnostic equipments. Moreover, the use of a Multislice Computed Tomography Angiography allows investigation of all aspects 82 CCM — Scientific Report 2011 — Ongoing research 2012 of vascular beds and body, particularly heart coronary arteries. The vascular patient is often affected by multiple disease processes and the optimal care is provided in a true interdisciplinary environment. Since its birth in 1982, Centro Cardiologico Monzino has always been focused on the cooperation between surgeons and cardiologists. Our accurate preoperative cardiac screening prior to vascular surgery allows us to reduce the risk to develop cardiac complications, lowering to 1% the risk of acute myocardial infarction in major vascular interventions. Patients suffering from cardiovascular pathologies usually undergo electrocardiogram (ECG) and transthoracic Doppler echocardiography. Should these tests be positive, a Dobutamine echo stress test is performed by a cardiologist. We routinely perform echo-stress test in patients older than 70 years because coronary artery disease (CAD) risk is high and echo-stress test has good accuracy in the identification of patients with significant angiographic CAD. Patients with a previous history of coronary artery disease, symptoms related to CAD or electrocardiography/ echocardiography/stress test abnormalities are evaluated with coronary angiography. Patients without echocardiography/ stress test abnormalities are considered eligible for surgery. Once patients at risk of cardiac disease have been identified, the appropriate medical or surgical therapy has to be started before vascular surgery. During the last year, in addition to the clinical activity, our Unit has been involved in different research activities. Important studies have focused on the composition of atherosclerotic thrombus in abdominal artery aneurysm as well as on the alteration of gluco and proteoglycans in the artery wall. Moreover, the analysis of oxidative stress role in patients undergoing carotid artery stenting vs carotid artery tromboendoarterectomy is ongoing; the Unit has also developed a study concerning the absorption of mesoglycans in vein wall extracellular matrix after oral administration. In the years to come the Vascular and Endovascular Surgery Unit will be focused on the development of a minimally invasive vascular pathologies endoscopic treatment project in order to reduce patient surgical trauma. 308 206 Particular attention is dedicated to the vascular and diabetic wound management. Vascular ulcers are often chronic and recurrent thus causing a considerable amount of morbidity among patients with peripheral vascular diseases, including work incapacity. The vascular foot lesions are treated with endovascular and/or surgical procedures. Moreover tissue substitutes – like engineered tissue – are used for peripheral lesions. exposure during thoracic endovascular aneurysm repair and subsequent follow-up. Eur J Cardiothorac Surg. 2012 (Epub ahead of print) Publications Dainese L, Guarino A, Burba I, Esposito G, Pompilio G, Polvani G, Rossini A. Heart valve engineering: decellularized aortic homograft seeded with human cardiac stromal cells. J Heart Valve Dis. 2012;21(1):125-34 Agrifoglio M, Zoli S, Cappai A, Trabattoni P, Spirito R, Biglioli P. Endovascular Treatment of Abdominal Aortic Aneurysm After Previous Left Pneumonectomy: A Sound Choice. Ann Vasc Surg. 2011;25(4):556e7-10 Zoli S, Trabattoni P, Dainese L, Annoni A, Saccu C, Fumagalli M, Spirito R, Biglioli P. Cumulative radiation Camera M, Brambilla M, Facchinetti L, Canzano P, Spirito R, Rossetti L, Saccu C, Di Minno MN, Tremoli E. Tissue factor and atherosclerosis: not only vessel wall-derived TF, but also platelet-associated TF. Thromb Res. 2012;129(3):279-84 Dainese L, Biglioli P. Human or animal homograft: could they have a future as a biological scaffold for engineered heart valves? J Cardiovasc Surg (Torino). 2010;51(3):449-56 CCM — Scientific Report 2011 — Ongoing research 2012 83 Cardiovascular Surgery Area Anaesthesiology and Intensive Care Unit Anaesthesiology and Intensive Care Unit 2011 Erminio SISILLO, MD Director Co-director: Luca Salvi, MD STAFF Deputy Directors: Claudio Brambillasca, MD, Sebastiana Gregu, MD, Glauco Juliano, MD, Valeria Mazzanti, MD, Guido Merli, MD, Stefano Salis, MD Assistants: Cristina Beverini, MD, Paola Moliterni, MD, Nora Piazzoni, MD, Paola Suriano, MD Head Nurse: Pierangela Andreoletti Nurses: Sonia Giulia Bianchi, Francesca Caggia, Herrera Nancy Acenelia Camacho, Domenico Cavagnuolo, Hassan Charoub, Paolo Crippa, Vito Cucchiara, Domenica D’Ambrosio, Aurelio Della Corte, Cristiane Dias, Lucia Di Palo, Giulio Orlando Fabbrizi, Sandra Faini, Silvana Falchi, Claudio Fedele, Veronica Giurgila, Pavel Alin Huci, Dagmar Lukovska, Laura Mantoan, Valeriu Ciprian Palamariu, Marques Carla Simone Palmeira, Alessandra Pappalettera, Luana Lucia Pellegrino, Valencia Maximo Rodriguez, Garcia Pilar Guadalupe Valverde Secretary: Rosalba Lamanna 84 CCM — Scientific Report 2011 — Ongoing research 2012 Cardiac and vascular operations Intensive Care Unit Off-site anaesthetic procedures Consultations N° Procedures 1200 850 510 1400 Activities 2011. The anaesthesiology team is involved, on daily-basis, in case assessment together with cardiologists and surgeons. Our Unit has developed different techniques of anaesthesia according to different kinds of surgery. In particular, anaesthetists take care of patient health conditions in the postoperative Intensive Care Unit, including 11 well-equipped beds with advanced monitoring systems, in order to avoid any postoperative dangerous complications (acute renal injury, respiratory distress syndrome, cardiogenic shock) that may contribute to precipitate the heart workload. During the last years the Unit developed loco-regional anaesthesia techniques to be used in different settings, mainly involving spinal cord stimulation for refractory angina and pain related to peripheral vascular disorders. In association with general anaesthesia, some coronary artery bypass grafts were performed with high thoracic epidural anaesthesia in order to reduce the intra and postoperative cardiac stress, reduce pain and hospital length of stay. Moreover loco-regional anaesthesia is mainly used in vascular surgery to perform carotid endoarterectomy; since the patient is awake, it allows a continuous assessment of consciousness level during surgery. Furthermore the Unit has been one of the first in Italy to routinely apply transesophageal echocardiography in all cardiac and main vascular operations. All the staff members are able to evaluate cardiac anatomy and function and to properly assist the surgeons in the achievement of the best results. Last but not least, due to more and more sophisticated invasive cardiology techniques, a skilled anaesthetist has become mandatory in the catheterization laboratory, to guarantee an adequate hemodynamic condition and sedation. By the end of 2010, we provided computer-supported multimodal bed side monitoring for all patients. The surveillance software can facilitate therapeutic errors prevention, improve therapy management and help achieving a higher standard of care. Publications Sisillo E, Marenzi G. N-acetylcysteine for the prevention of acute kidney injury after cardiac surgery. J Clin Pharmacol. 2011;51(11):1603-10 Tamborini G, Muratori M, Maltagliati A, Galli CA, Naliato M, Zanobini M, Alamanni F, Salvi L, Sisillo E, Fiorentini C, Pepi M. Pre-operative transthoracic real-time three-dimensional echocardiography in patients undergoing mitral valve repair: accuracy in cases with simple vs. complex prolapse lesions. Eur J. Echocardiogr. 2010;11(9):778-85 Bartorelli AL, Andreini D, Sisillo E, Tamborini G, Fusari M, Biglioli P. Left main coronary artery occlusion after percutaneous aortic valve implantation. Ann Thorac Surg. 2010;89(3):953-5 Salvi L, Beverini C, Maniglia P, Piazzoni N. Le Catecolamine in cardiochirurgia sono un bene o un male? Min Anest. 2009;75 Suppl 1:475-476 Sisillo E, Ceriani R, Bortone F, Juliano G, Salvi L, Veglia F, Fiorentini C, Marenzi G. N-acetylcysteine for prevention of acute renal failure in patients with chronic renal insufficiency undergoing cardiac surgery: a prospective, randomized, clinical trial. Crit Care Med. 2008;36(1):338-40 CCM — Scientific Report 2011 — Ongoing research 2012 85 Cardiovascular Imaging Area The Cardiovascular Imaging Area is a diagnostic department including three main areas: Echocardiographic Laboratories, Cardiovascular Radiological Imaging (Computed Tomography) and Cardiac Magnetic Resonance. It is an academic department with about 80 employees including cardiologists, radiologists and bioengineers dedicated to clinical, educational and scientific activities. Centro Cardiologico Monzino has an agreement with the Faculty of Medicine and the Cardiology and Radiology Postgaduate Schools of the University of Milano, and a convention with the Bioengineering Department of the Politecnico of Milano closely cooperating with us. The department has the most updated imaging techniques in the three areas: 21 ultrasound units (6 portable and 3 in the operating rooms) including three 3D echomachines, six transesophageal probes (one real time 3D probe), echo-stress, echo-contrast and DTI modalities, intracardiac echocardiography. In the Radiology Unit a 64 Cardiac CT is mainly dedicated to cardiac imaging activities (using the most advanced technologies to reduce radiation dose exposure as prospective ECG gating and new post-processing software). Cardiac Magnetic Resonance (“MR450 Discovery” with the magnetic field of 1.5 Tesla and 8-channels gradient coils) is performed by a dedicated unit equipped with all main cardiovascular tools. Portable echocardiographic units allow diagnostic procedures in the Emergency Unit, Intensive Cardiac Care Unit, catheter interventional and electrophysiological laboratories, as well as emergency echocardiograms in all the wards of the hospital. Main diagnostic procedures include: standard echocardiograms, echo-stress, echocontrast, transesophageal echocardiography, 3D echocardiography, intraoperative echocardiography, intracardiac echocardiography, cardiac computed tomography of the coronary arteries, cardiac chambers and peripheral vessels. Clinical activities are not only 86 CCM — Scientific Report 2011 — Ongoing research 2012 Mauro PEPI, MD Area Coordinator related to all cardiovascular pathologies in the workup of different main diagnostic-clinical protocols (approximately 130 main diagnostic work up protocols in congenital, acquired chronic or acute cardiovascular diseases), but also to several monitoring procedures (percutaneous procedures in the catheterization and EPS laboratories, intraoperative monitoring of percutaneous/ transapical aortic valve implantation, percutaneous pericardiocentesis). An integrated imaging approach (standard echo and echo-stress and/or cardiac CT, echo and cardiac CT, intracardiac echo and CT, CMR) is further improving the diagnostic work-up in new procedures. Several clinical and research protocols, closely related to new advanced techniques, have been activated trying to better demonstrate the role of 3D imaging in several pathologies (valve disease, congenital heart diseases) and the importance of dose radiation reduction in cardiac CT. As concerns this latest advancement in cardiac CT, new software allow a marked reduction in the radiation doses maintaining feasibility, definition and diagnostic accuracy of the technique. Cardiac Magnetic Resonance program further reinforces the concept of an integrated approach to cardiovascular pathologies, particularly in the field of cardiomyopathies, cardiac ischemia, valvulopathies, congenital heart diseases. CMR offers the unique advantage to evaluating all cardiac chambers with high spatial and temporal resolution in identifying (at rest and during pharmacologic stress) myocardial characteristics (thickness, viability, scars, perfusion). Moreover, precise measurements of right and left ventricular volumes and cardiac output facilitate quantitative evaluation of cardiac diseases. There is an excellent collaboration with all the other units within the frame of disease-specific multidisciplinary teams as it can be seen from the distribution of the diagnostic equipments, staff training and presence in all departments. The complexity of the link between clinical activities of the staff inside the core laboratories and inside the different wards (including emergency rooms, operating theatre, catheterization laboratories) reflects the evolving role of both the cardiologist who (except the interventional cardiologist) is deeply involved in imaging techniques and the radiologist dedicated to cardiovascular diseases. This is why in our units cardiologists and radiologists fully collaborate in several activities and a new type of cardiologist also trained (or specialized) in radiology has been introduced. More recently translational research projects have been implemented thanks to several collaborations with engineers. CCM — Scientific Report 2011 — Ongoing research 2012 87 Cardiovascular Imaging Area Echocardiography Unit Echocardiography Unit 2011 N° Procedures Total echocardiographic exams 23631 In-hospital exams 13351 Outpatients exams 10280 Transesophageal echocardiographic exams 1220 Stress echocardiographic exams 1383 3D-exams 620 Mauro Pepi, MD Director FULL-TIME STAFF Senior Deputy Directors: Paolo Barbier, MD, Claudia Galli, MD, Anna Maltagliati, MD, Gloria Tamborini, MD Assistant: Paola Gripari, MD Fellows: Claudia Cefalù, MD, Sarah Ghulam Ali, MD Bioengineers: Laura Fusini, Francesco Maffessanti, Federico Veronesi Head Nurse: Laura Carparelli Nurses: Dos Reis Satildes, Raffaella Fasso, Michela Ferrantino, Laura Fumagalli, Maria Gagliardo, Maria Salvatrice Giuttari, Rosanna Guadagno, Romina Locatelli, Maria Labori, Giuseppina Manca, Concetta Maiorana, Ennia Manoni, Inmaculada Marin Blanco, Donatella Miodini, Sandra Robledo, Alessandra Sartori, Enza Stefanizzi, Sabrina Zonelli Secretaries: AnnaMaria Bellavia, Salvina Comignolo PART-TIME STAFF Deputy Directors: Marina Alimento, MD, Fabrizio Celeste, MD, Elisabetta Doria, MD, Gianfranco Lauri, MD, Manuela Muratori, MD, Gianluca Pontone, MD Assistants: Daniele Andreini, MD, Giovanni Berna, MD, Jenesse Campodonico, MD, Gaia Cattadori, MD, Alessandra Magini, MD, Marco Matturri, MD, Francesca Susini, MD 88 CCM — Scientific Report 2011 — Ongoing research 2012 Activities 2011. Main diagnostic procedures include: standard echocardiograms, echo-stress, echo-contrast, transesophageal echocardiography, 3D echocardiography, intraoperative echocardiography, intracardiac echocardiography. Clinical activities are not only related to all cardiovascular pathologies in the work-up of different main diagnostic-clinical protocols (approximately 130 main diagnostic work up protocols in congenital, acquired chronic or acute cardiovascular diseases), but also to several monitoring procedures (percutaneous procedures in the catheterization and EPS laboratories and intraoperative monitoring of percutaneous/transapical aortic valve implantation, percutaneous pericardiocentesis). Emergency echo by portable ultrasound machines is frequently performed in all wards of the institute (approximatively 1000 / year). Main research activities Transthoracic 3D echocardiography Transesophageal 3D echocardiography Mitral valve prolapse and mitral valve repair Advancements in mitral valve annulus 3D reconstruction Advancements in aortic-mitral coupling through 3D reconstruction Left ventricular 3D shape in normal and pathological hearts Right ventricular systolic function Prosthetic valve dysfunction New insights into left atrial function New insights into transcatheter aortic valve implantation through combined 3D echo and CT approaches (prediction of post-TAVI aortic regurgitation, evaluation of aortic annulus, imaging of the coronary ostia, postTAVI LV systolic function) CCM — Scientific Report 2011 — Ongoing research 2012 89 Cardiovascular Imaging Area Magnetic Resonance Imaging Unit Gianluca PONTONE, MD Director STAFF Senior Assistant: Daniele Andreini, MD Assistant: Paola Gripari, MD Fellow: Erika Bertella, MD Residents: Sarah Cortinovis, MD, Saima Mushtaq, MD Chief Technician: Giuseppe Squilla Deputy Chief Technician: Claudia Daniela Foti Technicians: Alessandro Agozzino, Lorenzo Bonfanti, Giorgio Missana, Marisa Mu Head Nurse: Laura Carparelli Nurses: Edoarda Baraggia, Carmen Cinieri, Michela Ferrantino, Raffaela Putignano, Raffaella Sasso, Catia Trudu Secretaries: Emanuela Acanfora, Naty Mariconti, Massimo Vanni 90 CCM — Scientific Report 2011 — Ongoing research 2012 Activities 2011. In October 2010 the scanner MR450 Discovery with a magnetic field of 1.5 Tesla and 8-channels gradient coils was installed in our hospital. This platform is one of the few developed and used in the world mainly dedicated to cardiovascular applications and providing a high image quality in these clinical settings. The magnetic resonance (MRI) is one of the most recent and innovative diagnostic methods in the field of cardiac diseases. In this context, the main applications are accurate and reliable assessments of ventricular volumes, ejection fraction and ventricular myocardial mass, using techniques already in use in echocardiography, but with a greater definition of the endocardial and epicardial contours. Thanks to its excellent reproducibility, MRI can now be considered the gold standard for studies of myocardial perfusion and contractile reserve and for studies of myocardial viability by identifying areas of scarring of the myocardial wall, which today represent a milestone for indication of revascularization procedures and for prognostic stratification of patients with cardiac disease. MRI can be used in many clinical settings such as coronary artery disease, dilated cardiomyopathy, myocarditis, hypertrophic cardiomyopathy, arrhythmogenic right ventricular disease, congenital heart disease, valvular disease, pericardial disease and study of cardiac masses. In addition, MRI is a valid alternative to MDCT in the evaluation of vascular disease without the use of ionizing radiation and therefore with a higher safety for repeatability in patients requiring long and regular follow-up. The clinical activity includes 8 cardiovascular MRI each day, 50% scheduled for outpatients. The exams are performed by physicians with experience in cardiovascular imaging including echocardiography and cardiovascular multidetector computed tomography. Last year, 856 cardiovascular MRI and 194 stress cardiac MRI were performed. The three main indications were 1) coronary artery disease assessment (20%) 2) left atrium evaluation in patients undergoing pulmonary veins ablation for atrial fibrillation (13%) 3) ventricular arrhythmias (11%). The main research activities include applications in the field of aortic annulus evaluation in patients undergoing transaortic valve implantation, MRI-guided transcatheter atrial fibrillation and dilated cardiomyopathy. About the latter point, our Unit, in cooperation with the Electrophysiology Unit, has been chosen as core-lab for the international multicenter trial EMOSSID on the use of cardiac MRI as gatekeeper for intracardiac defibrillator device. Finally two international multicenter trials have been started: CMR-BLOOD in cooperation with the University of Los Angeles and Myocardial Salvage Trial with the CNR of Pisa. CCM — Scientific Report 2011 — Ongoing research 2012 91 Cardiovascular Imaging Area Radiology Unit Radiology Unit 2011 Giovanni BALLERINI, MD Director STAFF Senior Deputy Director: Enrica Maria Nobili, MD, Gianluca Pontone, MD Senior Assistant: Daniele Andreini, MD Assistants: Andrea Annoni, MD, Alberto Formenti, MD Fellows: Erika Bertella, MD Residents: Francesca Besana, MD, Sarah Cortinovis, MD, Saima Mushtaq, MD Chief Technician: Giuseppe Squilla Technicians: Alessandro Agozzino, Lorenzo Bonfanti, Patrizia Bravi, Roberto Casalino, Elisa Consiglio, Claudia Daniela Foti, Giorgio Missana, Marisa Mu, Antonietta Porru Nurses: Edoarda Baraggia, Carmen Cinieri, Raffaela Putignano, Catia Trudu Secretaries: Naty Mariconti, Massimo Vanni 92 CCM — Scientific Report 2011 — Ongoing research 2012 N° Procedures Cardiac computed tomographies 1800 Aortic and vascular computed tomographies 3600 Radiological evaluations 21000 Ultrasound examinations 2500 Activities 2011. Since 2004 the high level of collaboration between physicians and the administration management, has allowed the achievement of a high quality level in cardiovascular radiological diagnostic methods, particularly in cardiac Multi Detector Computed Tomography (MDCT). In the Radiology Unit, a 64-slice cardiac MDCT has been mainly dedicated to cardiovascular imaging activities, using both the most advanced technologies to reduce radiation dose exposure while maintaining feasibility, definition and diagnostic accuracy, and the most innovative post-processing software. In January 2010, the new CT-Scan Discovery 750HD was installed. In 2011 and early 2012 new software programs were developed allowing both an improvement of the time and space quality of images and a further reduction of the dose delivered to the patient in vascular exams. Together with the MDCT development, the traditional radiology has been modified thanks to the transformation of all diagnostics in computerized RX and to the consolidation of the PACS (Picture Archive and Communication System) which allows a realtime availability of the exams with an efficient interfacing with other diagnostic and care Units of the Institute. The ultrasound colordoppler imaging system allows diagnostic examinations in aortic and splanchnic vascular pathologies also thanks to the recent progress of studies with echo-contrast agents. Research is fully integrated with the daily clinical activity. In 2011 the main activity of MDCT was focused not only on coronary MDCT in patients with low-tointermediate pre-test risk and in patients affected by dilated cardiomyopathy, but also on the evaluation of revascularized patients (coronary artery bypass e coronary stents) and on different topics related to prognostic evaluation in patients who executed cardiac MDCT. Several studies were carried out to assess the feasibility and precision of MDCT exams performed by using new low dose protocols. Moreover about prognostic role of CT coronary angiography in patients with suspected coronary artery disease followed for 5 years, was concluded. We have developed a diagnostic MDCT pre-procedural method to be applied in transcatheter aortic valve substitutions carried out with a transfemoral or cardiac transapical approach. We are continuing the MDCT evaluation of sovra-aortic vessels and intracranial circulation in patients to be submitted to recanalization procedures and the preprocedure grading and follow-up in patients with aortic pathology and endoprosthesis implantation. Due to the fact that ultrasound investigation is non invasive, specific attention has been dedicated to this technique especially with regard to the renal arteries in patients with suspected nephrovascular arterial hypertension. The Unit is engaged in educational programs, organizing scientific meetings and theoretical and practical courses on cardiac MDCT and vascular Doppler ultrasonography. CCM — Scientific Report 2011 — Ongoing research 2012 93 Cardiovascular Imaging Area Publications. Pontone G, Andreini D, Bartorelli A, Cortinovis S, Mushtaq S, Bertella E, Annoni A, Formenti A, Nobili E, Trabattoni D, Montorsi P, Ballerini G, Agostoni P and Pepi M. Diagnostic accuracy of coronary computed tomography angiography. A comparison between prospective and retrospective electrocardiogram triggering. J Am Coll Cardiol 2009; 54: 346-355 Tamborini G, Ajmone Marsan, N, Gripari P, Maffessanti F, Brusoni D, Muratori M, Caiani E, Fiorentini C, Pepi M. Reference values for right ventricular volumes and ejection fraction with real-time three-dimensional echocardiography: evaluation in a large series of normal subjects. J Am Soc Echocardiogr 2010; 23: 109-115 Pepi M, Evangelista A, Nihoyannopoulos P, Flachskampf F, Athanassopoulos G, Colonna P, Habib G, Ringelstein E, Sicari R, Zamorano J on behalf of the European Association of Echocardiography. Recommendations for echocardiography use in the diagnosis and maanagement of cardiac sources of embolism. Eur J Echocard 2010; 11: 461-476 Maffessanti F, Caiani EG, Tamborini G, Muratori M, Sugeng L, Weinert L, Alamanni F, Zanobini M, Mor-Avi V, Lang RM, Pepi M. Serial Changes in Left Ventricular Shape Following Early Mitral Valve Repair.. Am J Cardiol 2010; 106(6):836-42 Ajmone Marsan N, Maffessanti F, Tamborini G, Gripari P, Caiani E, Fusini L, Muratori M, Zanobini M, Alamanni F, Pepi M. Left atrial reverse remodeling and function imporvement after mitral valve repair in degenerative mitral regurgitation: A real-time 4-dimensional echocardiographyy study. Am Heart J 2011; 161: 314-321 Ewe SH, Muratori M, Delgado V, Pepi M, Tamborini G, Fusini L, Klautz RJ, Gripari P, Bax JJ, Fusari M, Schalij MJ, 94 CCM — Scientific Report 2011 — Ongoing research 2012 Ajmone Marsan N. Hemodynamic and Clinical Impact of Prosthesis-Patient Mismatch After Transcatheter Aortic Valve Implantation. J Am Coll Cardiol. 2011;58(18):1910-1918 Pontone G, Andreini D, Bartorelli AL, Bertella E, Mushtaq S, Cortinovis S, Chiappa L, Annoni A, Formenti A, Trabattoni D, Montorsi P, Ballerini G, Fiorentini C, Pepi M. Comparison between low-dose multidetector computed coronary angiography and myocardial perfusion imaging test in patients with intermediate pretest likelihood of coronary artery disease. Int J Cardiol 2011; 147(3):454-457 Andreini D, Pontone G, Bartorelli AL, Mushtaq S, Trabattoni D, Bertella E, Cortinovis S, Annoni A, Formenti A, Ballerini G, Agostoni P, Fiorentini C, Pepi M. High diagnostic accuracy of prospective ECG-gating 64-slice computed tomography coronary angiography for the detection of in-stent restenosis : In-stent restenosis assessment by low-dose MDCT. Eur Radiol 2011; 21(7):1430-1438 Pontone G, Andreini D, Bartorelli AL, Annoni A, Mushtaq S, Bertella E, Formenti A, Cortinovis S, Alamanni F, Fusari M, Bona V, Tamborini G, Muratori M, Ballerini G, Fiorentini C, Biglioli P, Pepi M. Feasibility and accuracy of a comprehensive multidetetctor computed tomography acquisition for patients referred for balloon-expandable transcatheter aortic valve implantation. Am Heart J 2011;161:1106-1113 Pontone G, Andreini D, Bartorelli L, Bertella E, Mushtaq S, Annoni A, Formenti A, Chiappa L, Cortinovis S, Baggiano A, Conte E, Bovis F, Veglia F, Foti C, Ballerini G, Fiorentini C, Pepi M. Radiation dose and diagnostic accuracy of multi detector computed tomography for the detection of significant coronary artery disease: a metaanalysis. Int J Cardiol 2011; [Epub ahead of print] Montorsi P, Caputi L, Galli S, Ciceri E, Ballerini G, Agrifoglio M, Ravagnani P, Trabattoni D, Pontone G, Fabbiocchi F, MD, Loaldi A, Parati E, Andreini D, Veglia F, Bartorelli AL. Microembolization during carotid artery stenting in patients with high-risk, lipid-rich plaque. J Am Coll Cardiol 2011;58:1656–1663 Pontone G, Andreini D, Bartorelli AL, Bertella E, Mushtaq S, Foti C, Formenti A, Chiappa L, Annoni A, cortinovis S, Baggiano A, Conte E, Bovis F, Veglia F, Ballerini G, Agostoni PG, Fiorentini C, Pepi M. Feasibility and diagnostic accuracy of a low radiation exposure protocol for prospective ECG-triggering coronary MDCT angiography. Clin Radiol 2011; 67(3):207-215 Fusini L, Tamborini G, Gripari P, Maffessanti F, Mazzanti V, Muratori M, Salvi L, Sisillo E, Caiani EG, Alamanni F, Fiorentini C, Pepi M. Feasibility of Intraoperative ThreeDimensional Transesophageal Echocardiography in the Evaluation of Right Ventricular Volumes and Function in Patients Undergoing Cardiac Surgery. J Am Soc Echocardiogr. 2011;24(8):868-877 Sagit Ben Zekry, Robert M Saad, Mehmet Özkan, Maie S Al Shahid, Mauro Pepi, Manuela Muratori, Jiaqiong Xu, Stephen H Little, William A. Zoghbi. Flow Acceleration Time and Ratio of Acceleration Time to Ejection Time for Prosthetic Aortic Valve Function. J Am Coll Cardiol Img, 2011; 4:1161-1170 Lang RM, Badano LP, Tsang W, Adams DH, Agricola E, Buck T, Faletra FF, Franke A, Hung J, Pérez de Isla L, Kamp O, Kasprzak JD, Lancellotti P, Marwick TH, McCulloch ML, Monaghan MJ, Nihoyannopoulos P, Pandian NG, Pellikka PA, Pepi M, Roberson DA, Shernan SK, Shirali GS, Sugeng L, Ten Cate FJ, Vannan MA, Zamorano JL, Zoghbi WA. EAE/ASE Reccomendations for image acquisition and display using three-dimensional echocardiography. J Am Soc Echocardiogr. 2012;25(1):3-46 CCM — Scientific Report 2011 — Ongoing research 2012 95 Laboratory Medicine Unit Annalisa CAVALLERO, MD, Ph.D Director STAFF Deputy Director: Monica Raggi, DSc Assistants: Tiziana D’Errico, MD, Giovanni Introcaso, DSc, Daniela Riggio, DSc, Maria Rossi, MD, Roberta Temporiti, DSc (Alessandra Ratto, MD) Chief Technician: Paola Rumi Technicians: Chiara Ardeleani, Laura Cadau, Carmela Calvara, Cristina Frassi, Vanessa Guerra, Chiara Miggiano, Massimo Moreo, Giorgia Piras, Carmen Riva, Lorenza Rondelli, Simona Sabella 96 CCM — Scientific Report 2011 — Ongoing research 2012 Activities 2011. The Laboratory Medicine Unit encompasses the fields of biochemistry, coagulation, haematology, infectious disease serology, cancer markers, drug monitoring and microbiology. It serves both in and outpatients, and is also carrying out diagnostic laboratory tests for other hospitals or medical centres. Clinical chemistry and immunochemistry sections are integrated and equipped with recent and updated analyzers providing the best analytical and clinical performance. The coagulation section is certified for oral anticoagulant monitoring in patients who undergo a long-term therapy; the haematology section provides a first step screening on patients admitted to the hospital needing to undergo cardiovascular surgery. The microbiology section, besides carrying out tests on in and outpatients, performs culture tests for the Istituto Neurologico Besta and particularly for the ICU and neurosurgery departments. It also performs the microbiological tests required for the activity of the Cardiovascular Tissue Bank located at Centro Cardiologico Monzino by assessing tissue sterility before and after disinfection and by performing environmental controls to satisfy the requirements for tissue sterile preparations. The total number of tests carried out during 2011 was about 1.100.000. Moreover, the Unit organizes the supply of blood products by means of a dedicated team. The laboratory staff is composed of a team working very well together that meets and contacts daily the physicians of the hospital departments, resulting in a thorough vision of the patient health. The daily internal quality controls, and the involvement in external quality assessment programmes, either organized by Regione Lombardia or by private companies, guarantee the reliability of the test results. An updated online computerized system connects the lab with the wards, so that the results of the tests are rapidly available for the physician, immediately after validation. There is also an epidemiology programme that supplies the Infection Control Committee with the results of the microbiological research of the Institute. Moreover, the medical staff of the laboratory, in association with FCSA (Federazione Centri per la diagnosi della trombosi e la Sorveglianza delle terapie Antitrombotiche), is in charge of the supervision of the oral anticoagulant therapy to outpatients. Besides traditional diagnostic laboratory tests, the Unit is involved in a research project on the evaluation of new cardiac biomarkers in suspected acute coronary syndrome (ACS) in collaboration with the Coronary Care Unit. Furthermore, the laboratory collaborates with other groups of Centro Cardiologico Monzino and other hospitals in Milano on several research projects and clinical trials. Publications Cattadori G, Wasserman K, Meloni C, Mustaq S, Contini M, Apostolo A, Andreini D, Magrì D, Sciomer S, Veglia F, Berna G, Introcaso G, Palermo P, Fiorentini C, Agostoni P. Alveolar membrane conductance decreases as BNP increases during exercise in heart failure. Rationale for BNP in the evaluation of dyspnea. J Card Fail. 2009;15(2):136-44 CCM — Scientific Report 2011 — Ongoing research 2012 97 Introcaso G, Raggi M, D’Errico T, Cavallero A. Shortterm increases of plasma cardiac troponin I are better evaluated by comparison with the reference change value. Biochemia Medica 2010;20(3):327-33 Marenzi G, Giorgio M, Trinei M, Moltrasio M, Ravagnani P, Cardinale D, Ciceri F, Cavallero A, Veglia F, Fiorentini C, Cipolla CM, Bartorelli AL, Pelicci P. Circulating cytochrome c as potential biomarker of impaired reperfusion in ST-segment elevation acute myocardial infarction. P. Am J Cardiol. 2010;106(10) 98 CCM — Scientific Report 2011 — Ongoing research 2012 Marenzi G, De Metrio M, Rubino M, Lauri G, Cavallero A, Assanelli E, Grazi M, Moltrasio M, Marana I, Campodonico J, Discacciati A, Veglia F, Bartorelli AL. Acute hyperglycemia and contrast-induced nephropathy in primary percutaneous coronary intervention. Am Heart J. 2010;160(6):1170-7 Research Laboratories Gatti S, Rama P, Matuska S, Berrilli F, Cavallero A, Carletti S, Bruno A, Maserati R, and D Di Cave J. Isolation and genotyping of Acanthamoeba isolates from corneal infections in Italy. Med. Microbiol. 2010;5: 1324-30 CCM — Scientific Report 2011 — Ongoing research 2012 99 Laboratory of Biology and Biochemistry of Atherothrombosis (4 Units) Elena TREMOLI, Ph.D Director Alessandro PAROLARI, MD, Ph.D Deputy Director Head of the Clinical Research Unit 1. Marina Camera, Ph.D Head of the Unit of Cell Biology and Biochemistry of Atherothrombosis 2. Cristina BANFI, Ph.D Head of the Unit of Cardiovascular Proteomics 3. Viviana Cavalca, Ph.D Head of the Unit of Biochemistry of Oxidative Stress and Endothelial Function in Atherothrombosis Activities 2011. The main goals of the laboratory are: •to understand how cardiovascular system responds to physiological and pathological changes •to identify new biomarkers of cardiovascular diseases •to develop new therapeutic approaches Within the laboratory there are 4 units of research, which strictly cooperate with clinical researchers to develop both basic and translational research. 4. Luigi Sironi, Ph.D Head of the Unit of Experimental Thrombosis and Imaging in vivo 100 CCM — Scientific Report 2011 — Ongoing research 2012 CCM — Scientific Report 2011 — Ongoing research 2012 101 1. Unit of Cell Biology and Biochemistry of Atherothrombosis Marina CAMERA, Ph.D Head of the Unit STAFF Daniela Boselli, PhD Marta Brambilla, PhD Laura Facchinetti, PhD student Laura Rossetti, PhD student Paola Canzano, MSc Franco Moro, Technician Activities 2011. The research activities performed by the Unit of Cell Biology and Biochemistry of Atherothrombosis are focused on the biochemical, cellular and molecular mechanisms involved in the development and progression of the atherothrombotic disease and on their pharmacological modulation. To this aim, the Unit uses approaches ranging from cell biology to molecular biology, with a highly integrated strategy between basic (using both in vitro cultures of human and animal cells, animal models) and clinical research performed on patients with cardiovascular disease. Furthermore, a genomic and proteomic approach is also exploited in order 1) to study the mechanisms of regulation and the pharmacological modulation of key proteins involved in thrombotic processes; 2) to identify genes and proteins with altered expression in cells, tissue or biological fluids of patients with cardiovascular diseases in order to discover new pathogenetic mechanisms as well as biomarkers able to predict the presence of disease at an early stage, the evolution of the disease, or the risk of clinical events; 3) to correlate the interindividual variation in response to drugs with polymorphisms in genes encoding target proteins (receptors, enzymes, ion channels) of drugs (pharmacogenetics) in order to tailor a personalized therapeutic intervention; 4) to identify the role of polymorphisms and/or mutations in proteins playing key roles within the atherothrombotic process (pharmacogenomics). All these research activities are performed in close collaboration with clinical units within the Centro Cardiologico Monzino. New pathogenetic mechanisms in acute coronary syndrome: platelet transcriptomic and proteomic analysis. Although platelets do not have a nucleus, they contain more than 2000 megakaryocyte-derived mRNAs, which may influence pathophysiological functions. Comparing the platelet transcriptome of SA and NSTE-ACS patients we identified 45 differentially expressed genes involved in 102 CCM — Scientific Report 2011 — Ongoing research 2012 signal transduction, macromolecular complex assembly, and response to stress that may modulate platelet reactivity in CAD. The analysis of the platelet proteome in SA and NSTE-ACS patients identified differential expression in proteins, not previously connected with CAD, such as energy metabolism enzymes, and proteins associated with cytoskeleton-based processes, both of which indicate platelet activation. New pathogenetic mechanisms in acute coronary syndrome: the role of platelet-associated Tissue Factor. Tissue Factor is a 47 kD glycoprotein which triggers the blood coagulation cascade. Its expression within the atherosclerotic plaque directly correlates with the plaque thrombogenicity. We previously described the presence of TF in human platelets and we showed that this glycoprotein is expressed under the control of both platelet agonists and of some antiplatelet drugs. Recently we provided the evidence that TF expression is significantly higher in resting platelets of patients with ACS than in patients with SA. This results in a higher capacity of platelet to generate thrombin, which in turn contributes to the prothrombotic phenotype of ACS patients. Chronic Kidney Disease in Acute Myocardial Infarction: platelet function assessment and platelet transcriptomic and proteomic analysis. Patients with chronic kidney disease (CKD) have a higher incidence of coronary artery disease (CAD). CKD causes modifications in platelet reactivity leading to a higher rate of thrombotic complications compared to CAD patients without CKD. The underlying mechanisms have not been clarified yet. Flow cytometric analysis of platelet and leukocyte activation showed a platelet- and platelet-monocyte CCM — Scientific Report 2011 — Ongoing research 2012 103 aggregates associated TF expression significantly lower in CAD patients with CKD than in those without CKD, both under basal conditions and after stimulation with ADP. The reduction of TF observed might be attributable to a continued consumption or release of TF-loaded microparticles in patients with CKD. The finding that after in vitro ADP stimulation only the expression of TF is significantly lower in patients with CKD would support this hypothesis. CAD/CKD platelets showed distinct transcript expression profiles compared to CAD. In addition, the expression level of several genes seemed to be influenced by the glomerular filtration rate. One molecular function, in particular, appeared to be affected by renal failure both in the SA and in the NSTE-ACS platelets: the regulation of actin cytoskeleton exerted by the integrin signaling pathway. Finally, also the proteomic study revealed that patients with CKD have a different plasma proteome pattern in respect to patients without CKD both in the stable angina and NSTEMI patients groups. Percutaneous coronary and carotid intervention and platelet activation. Drug-eluting stents (DES) are the treatment of choice in percutaneous coronary intervention (PCI). Concerns have been raised, however, about a possible association between DES and an increased late stent thrombosis rate. Dual antiplatelet therapy with aspirin and clopidogrel is the standard of care following DES implantation. Recently we showed that, despite the dual antiplatelet therapy, platelet activation in DES-treated patients is higher than in medically treated SA patients and further increases one month after thienopyridine discontinuation. Although the classical markers of platelet activation tended to those found in SA patients at 6 months after thienopyridine withdrawal, TF-positive platelets remained significantly higher than those of SA patients suggesting a direct implication for late DES thrombosis. Carotid Artery Stenting (CAS) is an evolving method to treat carotid stenosis. Platelet activation in CAS occurs 104 CCM — Scientific Report 2011 — Ongoing research 2012 as a result of vessel wall damage and subendothelium exposure leading to local thrombosis and distal embolization (periprocedural risk of temporary or permanent ischemic neurological deficits). The dual antiplatelet regimen (aspirin+thienopyridine) has a significant impact on reducing adverse neurological outcomes. Our studies evidenced a significant higher levels, compared to controls, of TF-positive platelets circulating in peripheral blood of CAS patients. Of note, dual antiplatelet therapy inhibits the expression of all ADP-induced platelet activation markers, but TF, thus suggesting that this prothrombotic platelet phenotype may have implications for CAS complications. Interindividual variation in the response to aspirin. Several studies have reported that aspirin sometimes fails to completely inhibit platelet function in patients with cardiovascular disease. The phenomenon, called “aspirin resistance”, may be due to several reasons, including alternative “upstream” pathways of platelet activation, as well as acquired or genetic factors. Moreover, the assessment of aspirin resistance is not simple because it is highly assay-dependent, and a general agreement on standardised, reproducible and specific tests to detect this phenomenon is still lacking. We performed two studies on this issue. The first one is a functional study in patients after coronary artery bypass graft (CABG), who are at high risk of adverse cardiovascular events, despite aspirin treatment; the second one was a pharmacogenetic study carried out in coronary disease patients. Our results indicate that, early after CABG, the incidence of aspirin resistance is lower in patients who received 325 mg aspirin compared to those who received 100mg ASA. Moreover, evidence is provided that different methods yield different results in the detection of aspirin resistance, rendering them not interchangeable. As far as the pharmacogenetic study is concerned, we assessed the influence of the GPIIb Ile843Ser SNP on the antiplatelet effects of ASA in 889 coronary disease patients (CHD) and found that residual platelet aggregation and TXB2 production in ASA-treated CHD patients differ between GPIIb Ile843Ser genotypes. Carriers of the Ile/Ile genotype may require higher doses of aspirin than Ser/ Ser patients to optimize anti-platelet therapy. Characterization of human atherosclerotic carotid plaque by histological techniques and multidetector computed angiography. Plaque morphology is an important predictor for the risk of stroke. Thus, it should be clinically relevant to be able to predict the risk of stroke based on plaque composition. Digital subtraction angiography (DSA) is the gold standard for the assessment of the degree of stenosis but it is unable to make any predictions about plaque composition. We carried out a study to determine the efficacy of multidetector computed tomography (MDCT) to characterize carotid atherosclerotic plaque morphology and composition as assessed by absolute quantitative analysis of histologic images using a dedicated software. We found a good correlation between histology and MDCT (K=0.76) indicating that MDCT angiography allows non-invasive assessment of the carotid plaque composition. TF SNPs and IMT. To Tissue Factor (TF), key initiator of coagulation, roles have been ascribed not only in thrombosis but also in atherosclerosis. TF gene promoter haplotypes modulate TF expression, thereby potentially affecting atherosclerosis. We have recently observed that the haplotype-tagging TF A-603G polymorphism is associated with carotid intima-media thickness, independently of TF levels in plasma, providing clinical evidence of an involvement of TF in atherosclerosis, in addition to its wellknown roles in haemostasis and thrombosis. Inflammation in CAD and in bypass complications. Inflammation plays a major role in the pathogenesis of atherosclerosis and particularly in the development of the vulnerable plaque. We reported that patients with a history of onset of CHD as an ACS display a significantly more intense serum amyloid A response to influenza vaccination, a non-vascular inflammatory stimulus, than patients with a history of onset of CHD as exercise-inducible myocardial ischemia, suggesting a pro-inflammatory status in patients prone to ACS but not in those with inducible myocardial ischemia. An inflammatory response is also induced by cardiopulmonary bypass in patients undergoing cardiac surgery. Our studies in this field indicate that, after coronary bypass surgery, there is a protracted postoperative activation of inflammation persisting several days after surgery; this postoperative activation is not affected by the surgical strategy (on-pump or off-pump). Publications Camera M, Brambilla M, Boselli D, Facchinetti L, Canzano P, Rossetti L, Toschi V, Tremoli E. Functionally active platelets do express tissue factor. Blood 2012; 119:4339-4341 Camera M, Brambilla M, Facchinetti L, Canzano P, Spirito R, Rossetti L, Saccu C, Di Minno MN, Tremoli E. Tissue Factor and Atherosclerosis: Not only vessel wall-derived TF, but also platelet-associated TF. Thromb Res. 2012;129(3):279-84 Capra V, Bäck M, Barbieri SS, Camera M, Tremoli E, Rovati GE. Eicosanoids and Their Drugs in Cardiovascular Diseases: Focus on Atherosclerosis and Stroke. Medicinal Research Reviews 2012 [Epub ahead of print] Di Minno MN, Guida A, Camera M, Colli S, Di Minno GD, Tremoli E. Overcoming limitations of current antiplatelet drugs: A concerted effort for more profitable strategies of intervention. Ann Med. 2011;43(7):531-44 Colombo G, Gertow K, Marenzi G, Brambilla M, De Metrio M, Tremoli E, Camera M. Gene expression profiling reveals multiple differences in platelets from patients with stable angina or non-ST elevation acute coronary syndrome. Thromb Res. 2011; 128(2): 161-168 CCM — Scientific Report 2011 — Ongoing research 2012 105 2. Unit of Cardiovascular Proteomics Cristina BANFI, Ph.D Head of the Unit STAFF Maura Brioschi, Ph.D Simona Cosentino, Ph.D Sabrina Lento, MSc Stefania Ghilardi, Technician Activities 2011. Proteomics, the study of an organism’s complete complement of proteins, is an emerging field that has the potential to uncover new therapeutic targets for the treatment and prevention of cardiovascular diseases, as well as new diagnostic biomarkers for early disease detection. Proteomicsbased studies are focused on the interactions of multiple proteins and their role as part of a biological system rather than the structure and function of one single component. Proteins are indeed directly involved in virtually all cellular activities and, as such, influence cell phenotype and hence the tissues and organs. This phenotype is the result of a dynamic, ongoing process of protein expression and modification and varies both under normal physiological conditions (e.g., cell-cycle stage, differentiation, function and age) or in response to pathophysiological stresses. Also environmental changes have the potential to alter protein structure and function, and may ultimately determine disease progression and outcome. Proteomic investigations in the field of cardiovascular disease involve the characterisation of these modifications in order to identify novel therapeutic targets and strategies to prevent the development of cardiovascular diseases. The goal of the Unit of Proteomics is the development of new, generally applicable technologies for proteomic analysis for generating new discoveries in specific areas of cardiovascular research using a synergistic combination of contemporary two-dimensional gel electrophoresis, a well established mass spectrometry facility, and state-of-the-art methods of biochemistry and gene expression/regulation analysis. Several proteomic approaches have been recently applied by the Laboratory of Proteomics to the study of: a) plasma; b) circulating cells; c) circulating mediators (lipoprotein, microparticles); d) secreted proteins (secretome); e) cell cultured systems; f) tissues; and 106 CCM — Scientific Report 2011 — Ongoing research 2012 g) organelles in the search for new mechanistic or diagnostic biomarkers for cardiovascular diseases. Plasma Proteome. The incorporation of proteomic analysis of plasma into functional biochemical and biological approaches can provide a powerful means of identifying patho/physiological pathways in cardiovascular diseases as it allows the simultaneous detection of different circulating proteins and their posttranslational modifications that cannot be identified by conventional measurements. We applied this approach to the investigation of the complex network of molecular mechanisms involved in the deleterious effects of coronary artery bypass graft (CABG) surgery and in coronary artery disease (CAD). In CABG we described an increase of α1-antichymotrypsin and cathepsin G levels which can reflect the generation of a proinflammatory and of a prothrombotic state remarking the significant involvement of neutrophil activation. Overall these data suggest potential new therapeutic targets which may help improving the results of this kind of surgery that, in recent years, has been offered to sickest patients who were earlier not considered to be good candidates or even unsuitable for surgery. Although the involvement of these pathways in the systemic stress response seems to be quantitatively and quantitatively important, its CCM — Scientific Report 2011 — Ongoing research 2012 107 role, the role of possible drug modulation and whether it is beneficial or not, needs further investigation in larger patient series. In addition, further studies are also needed to analyse the possible relevance and application of the different proteins as biomarkers of clinical prognosis. In CAD the proteomic study revealed that patients with chronic kidney disease (CKD) have a different plasma proteome pattern in respect to patients without CKD both in the stable angina and NSTEMI patients groups. Therefore, with the application of proteomic techniques, biomarkers can be identified without previous knowledge of their involvement in the pathogenesis of ACS, and its comorbidities, such as CKD. However, the field is in the early stages of evolution, and large-scale clinical studies are required to validate the usefulness of newly identified biomarkers in diagnosis, risk stratification, treatment and follow-up of cardiovascular diseases. Circulating cells represent an important target of proteomics because they can bear information reflecting directly an inflammatory or pro-coagulant state related to the pathology. We focused on the analysis of platelets whose participation in the genesis of chronic atherosclerotic lesions and the formation of thrombi that acutely occlude arteries, causing serious disease, is now well established. Furthermore, by understanding the multifaceted mechanisms involved in platelet interactions with vascular surfaces and aggregation, new approaches can be tailored to selectively inhibit the pathways most relevant to the pathological aspects of atherothrombosis. In this context, we observed that the platelet proteome is altered in patients with stable or acute coronary syndrome possibly as a consequence of the ongoing atherosclerotic process. The identified protein changes, not previously connected with coronary artery disease, were an increase in the energy metabolism enzymes, and alterations in the proteins associated with cytoskeleton-based processes, both of which indicate platelet activation. 108 CCM — Scientific Report 2011 — Ongoing research 2012 Circulating mediators: lipoprotein and microparticles. The mechanisms by which human low density lipoprotein LDL manifests its atherogenic properties have been, indeed, the topic of intense investigation during the past decades but, still, few data have been reported on proteins contained in human LDL and their possible functional roles. Lipoprotein particles are stabilized in the bloodstream by association with highly evolved proteins called apolipoproteins, which through lipidbinding regions containing both hydrophilic and hydrophobic surfaces facilitate binding between protein and phospholipids. These stabilizing proteins also mediate particle metabolism by binding to specific receptors on cell surfaces, as well as acting as cofactors for enzymes. For example, apoB-100 binds to arterial wall proteoglycans, promoting subendothelial retention of atherogenic LDL in early atherosclerosis. Besides known LDL-associated proteins, our proteomic analysis revealed the presence of proteins not previously described to reside in LDL, including prenylcysteine lyase (PCL1), orosomucoid, retinol-binding protein, and paraoxonase-1. Of interest, PCL1, an enzyme crucial for the degradation of prenylated proteins, generates free cysteine, isoprenoid aldehyde and hydrogen peroxide. The integration of the proteomic data with biochemical and gene expression analysis allowed us to assess that PCL1 is generated along with nascent lipoprotein and that it can itself generate an oxidant, thus suggesting that PCL1 may play a significant role in atherogenesis. Cellular microparticles (MP) are fragments shed from plasma membrane blebs of virtually all cell types when submitted to a number of stress conditions, including apoptosis. MP release is an integral part of the membrane-remodeling process in which the asymmetric distribution of constitutive phospholipids between the two leaflets is lost. MP have recently been shown to reflect in vitro cell stimulation, and testify to cellular activation and/or tissue degeneration occurring in vivo under a variety of pathophysiologic circumstances. Recent studies report the presence of endothelialderived MP in peripheral blood from patients with lupus anticoagulant, TTP, acute coronary syndromes, and even in blood of healthy individuals. Furthermore, we have recently demonstrated that cardiomyocytes release thrombogenic microparticles which in the setting of cardiac diseases might contribute to an increased thrombogenicity in the heart. Besides their characteristic markers, MP have been indeed identified as true vectors in the transcellular exchange of biologic information. In addition to their direct effect on the promotion and the amplification of the coagulation cascade, MP participate in a variety of intercellular adhesion processes and induce cellular responses. Functions of MP should be reflected by their protein composition, yet a comprehensive characterization of their antigenic composition is still lacking. Thus proteomic investigations are currently carried out to allow formal identification of endothelial cells- and cardiomyocytesderived microparticles proteins, offering the possibility to better understand their physiological role. The secretome, recently emerged as a new term to describe the global study of proteins that are secreted by a cell at any given time or under certain conditions, constitutes an important class of proteins that control and regulate a multitude of biological and physiological processes, thus making it a clinically relevant source for biomarkers and therapeutic target discoveries. In this respect, the application of a global proteomic approach to determine the effect of statins on the proteins released, “secretome”, by endothelial cells, could help to understand novel mechanisms by which statins promote some of their beneficial effects. The clinical benefits of 3-hydroxy-3-methyl-3-glutaryl coenzyme A (HMG-CoA) reductase inhibitors (statins) are strongly related to their low density lipoprotein-cholesterol lowering properties. However, because mevalonic acid, the product of HMG-CoA reductase reaction, is the precursor not only of cholesterol but also of nonsteroidal isoprenoid compounds, the inhibition of HMG-CoA reductase may result in pleiotropic effects. Indeed, a variety of experimental data indicates that statins can interfere with major events involved in the formation of atherosclerotic lesions, independently from their hypocholesterolemic properties, although these effects have not been fully elucidated. We are currently applying two methods for the identification and quantification of proteins differentially regulated by statins: the classical “gel based method” employing 2-DE, which offers the advantage to distinguish between proteins isoforms as well as different post-translationally modified forms of the same proteins, and a recently developed “gel-free MS-based method” for “label-free” quantitation, which provided absolute quantitative profiling of proteins. The results coming from the application of both approaches, validated by biochemical assays and gene expression analysis, will allow us to fully characterize the secretome of endothelial cells and to identify the drug-regulated proteins, and will have the potential to become a major focus of drug discovery programs throughout the industry. Proteomic analysis of in vitro cell systems. In the context of cellular proteome we are currently interested in the cellular phenotyping following gene silencing by RNAi. Systematic phenotyping by RNAi will provide new perspectives on gene function in the context of the genome on a gene-by-gene level and will allow to dissect many important cellular processes with an unprecedented spatial and temporal resolution. We are currently exploring the inhibition effect of the Tissue Factor (TF) expression by its specific siRNA in cardiomyocytes. The relevance of this issue arises from the observation that TF, switching the “on-off” of extrinsic coagulation cascade as the initiating factor, has been revealed presenting characteristics of signal receptor. TF-mediated CCM — Scientific Report 2011 — Ongoing research 2012 109 signaling was demonstrated to be intimately correlated with its nonthrombotic functions in tumor, angiogenesis and inflammatory. In the cardiovascular setting, TF is abundantly expressed by cardiomyocytes in the human heart where it is present in the transverse part of the intercalated disk and co-localizes with the cytoskeletal proteins. In patients with dilated cardiomyopathy, hypertension and ventricular hypertrophy, the TF level was found to be reduced in structurally altered ventricular myocardium. The reduction in TF expression and change in localization may influence cell-to-cell contact stability and contractility, thereby contributing to cardiac dysfunction in DCM. Nevertheless, it has not been completely elucidated how TF plays its role in maintaining the structural integrity and contractility of the myocardial muscle. The unexplored human mitral valve prolapse proteome. This translational research program is aimed to investigate the cellular and molecular regulators of tissue remodeling during the development of human Myxomatous Mitral Valve Prolapse (MVP), the most common indication for mitral valve surgery due to severe mitral regurgitation, by using merging proteomics and cellular biology approaches. Echocardiographically, MVP is defined as a single or bileaflet prolapse, at least 2 mm beyond the long-axis annular plane, with or without leaflet thickening. The prevalence of MVP is estimated at 2–3%, and is equally distributed between men and women. MVP is expected to occur in approximately 7.2 million individuals in the US, and over 144 million worldwide. Currently, no diagnostic or therapeutic approaches are available to identity patients at high risk of developing MVP and mitral regurgitation and/or to alter the progress of the disease. MV repair is the most accepted type of surgical intervention for severe MV regurgitation. The longevity of the repair, in experienced hands, is remarkable. The biomechanical forces present prior to the operation disappear 110 CCM — Scientific Report 2011 — Ongoing research 2012 postoperatively, and the valve dynamics are reset. The removal of these mechanical forces upon the valve leaflets in conjunction with a remodeling annuloplasty, allows for a significantly improved leaflet cooptation and valve performance. We could speculate that the removal of the previously present stress forces onto the valve leaflets is a fundamental factor in the resetting the normal valvular cellular physiology and directly responsible for the long-term durability of this type of operation. Therefore, merging proteomic approach to identify molecular determinants of MVIC cell biology with clinical studies will help to better understand when healthy quiescent MVICs get activated and start remodeling ECM leading to MVP development. Organelle proteomic. Focusing on specific organelle proteomes is an attractive alternative to reduce the tremendous complexity of the cellular/tissue proteomes and represents an attainable goal for better spatial and functional correlations of the identified proteins. In the organelle proteomic approach, the identified proteins come from distinct subcellular locations, which are often coupled with the biological processes in which they participate, thus providing the functional significance of proteomic data. To this regard, a subproteome analysis of caveolin-1 enriched membrane microdomains of human hearts allowed us to identify multiple proteins whose expression is altered in heart failure, thus opening new perspectives to determine which role they may play in this disease. Redox proteomics. The field of redox proteomics, although relatively new and rapidly changing, has the potential to revolutionize how we diagnose diseases, assess risks, determine prognoses, and target therapeutic strategies for people with cardiovascular diseases. Proteins are indeed the major targets for reactive oxygen species because of their abundance in biological systems and because they are primarily responsible for most functional processes within cells. Oxidative changes of protein structure are irreparable and can have a wide range of downstream functional consequences, such as inhibition of enzymatic and binding activities, increased susceptibility to aggregation and proteolysis, increased or decreased uptake by cells, and altered immunogenicity. That oxidation of proteins plays an essential role in the pathogenesis of an important number of degenerative diseases is now recognized. We applied a proteomic analysis focused at investigating the oxidative stress-induced modification of proteins in plasma of heart failure patients revealed the presence of specific targets whose biological activity is altered, alpha-1-antitrypsin and fibrinogen. Oxidation of alpha-1-antitrypsin resulted in loss of its protease inhibitor activity, thus leading to endothelial cell death. On the other hand, fibrinogen, when oxidized, became otherwise cytotoxic and induced apoptosis in endothelial cells. Overall our findings suggest that oxidised biomolecules are not only surrogate markers of oxidative stress, but may also play a role in the development of heart failure. More recently, we showed that oxidative stress-induced protein modifications are increased in the myocardium of patients with heart failure, and the proteomic approach made it possible to ascertain that two proteins mainly underwent carbonylation, M-type creatine kinase (M-CK), whose activity is impaired, and, to a lesser extent, α-cardiac actin. Exposure of cardiomyocytes to angiotensin II and norepinephrine led to mitochondrial ROS generation and M-CK carbonylation with loss of its enzymatic activity. Our findings indicate that protein carbonylation is increased in the myocardium during HF and that these oxidative changes may help to explain the decreased CK activity and consequent defects in energy metabolism observed in heart failure. Publications Banfi C, Brioschi M, Barcella S, Wait R, Begum S, Galli S, Rizzi A, Tremoli E. Proteomic analysis of human low-density lipoprotein reveals the presence of prenylcysteine lyase, a hydrogen peroxide-generating enzyme. Proteomics 2009; 9(5):1344-52 Banfi C, Parolari A, Brioschi M, Barcella S, Loardi C, Centenaro C, Alamanni F, Mussoni L, Tremoli E. Proteomic Analysis of Plasma from Patients Undergoing Coronary Artery Bypass Grafting Reveals a Protease/ Antiprotease Imbalance in Favor of the Serpin alpha1Antichymotrypsin. J Proteome Res. 2010;9(5):2347-57 Banfi C, Brioschi M, Marenzi G, De Metrio M, Camera M, Mussoni L, Tremoli E. Proteome of platelets in patients with coronary artery disease. Exp Hematol. 2010;38(5):341-50 Banfi C, Brioschi M, Lento S, Pirillo A, Galli S, Cosentino S, Tremoli E, Mussoni L. Statins prevent tissue factor induction by protease-activated receptors 1 and 2 in human umbilical vein endothelial cells in vitro. J Thromb Haemost. 2011;9(8):1608-19 Brioschi M, Polvani G, Fratto P, Parolari A, Agostoni P, Tremoli E, Banfi C. Redox Proteomics Identification of Oxidatively Modified Myocardial Proteins in Human Heart Failure: Implications for Protein Function. PLoS One. 2012;7(5):e35841 CCM — Scientific Report 2011 — Ongoing research 2012 111 3. Unit of Biochemistry of Oxidative Stress and Endothelial Function in Atherothrombosis Viviana CAVALCA, Ph.D Head of the Unit STAFF Sonia Eligini, Ph.D Isabella Squellerio, Ph.D Mauro Crisci, MSc Benedetta Porro, MSc Paola Songia, MSc Loredana Boccotti, Technician Activities 2011. Oxidative stress and endothelial dysfunction are considered important topics in the onset and progression of atherosclerotic and cardiovascular diseases. Oxidative stress is the result of the imbalance between the generation of free-radicals and the antioxidant defence system and has been related to physiological conditions, such as aging and physical activity, and to many chronic and degenerative pathologies. An important oxidant role has been ascribed to overproduction of free radicals, in particular reactive oxygen species (ROS). ROS are normal and beneficial products of oxidative cellular metabolism. These biochemically active free-radical derivatives of molecular oxygen act as normal signalling molecules in the vasculature; however, due to their reactivity, free radical can induce oxidative damage to proteins, lipids and DNA causing oxidative injury to vascular cells and promoting endothelial dysfunction. As a consequence, a diminished nitric oxide (NO) synthesis, an altered vasodilatation and an increased platelet aggregation could be observed. Besides endothelial cells, that are considered the major source of NO, circulating cells (erythrocytes, platelets and monocytes) are also able to synthesize NO. The contribution of red blood cells (RBC) to NO biosynthesis has been only recently highlighted. Our group has a long-standing interest in metabolic pathways involved in oxidative stress and NO synthesis. Thus the research activities of the Unit are focused on the study of oxidative stress in relation to endothelial dysfunction and activation of circulating blood cells, as platelets, leukocytes and red blood cells. In our Unit, chromatographic methods (HPLC, LC-MS/ MS) with high sensitivity and specificity have been set up in order to determine oxidative modifications of proteins, lipids and nucleic acids in plasma and urine. A pattern of antioxidant factors (vitamins, glutathione, antioxidant enzymes etc.) and the total antioxidant 112 CCM — Scientific Report 2011 — Ongoing research 2012 capacity can be measured. With regards to NO synthesis pathway, few studies have addressed the concomitant evaluation of the multiple aspects of NO pathway, also in consideration of the numerous compounds (substrate, cofactors and inhibitors) involved in its biosynthesis and metabolism. The introduction of innovative approaches for the comprehensive and quantitative analysis of wide arrays of metabolites has opened new perspectives for the understanding of these mechanisms in vivo. This emerging technology, called metabolomics, describes the biochemical pathways in terms of metabolites with low molecular weight present in cells, tissues, organs and biological fluids. The components of the metabolome can be detected as the end products of gene expression or protein activity (enzymes), thus defining the biochemical phenotype of a biological system as a whole. Our recent efforts have been focused to set up an LC-MS/MS method and detect Arginine/NO targeted metabolome in plasma and RBC. Currently, we measure the substrate, arginine, the inhibitors, symmetric- and asymmetric methylarginines (ADMA, SDMA) and the enzymatic cofactor, tetrahydrobiopterin. The metabolic products of arginine (ornitine and citrulline ) are also measured. During 2011 we have carried out several studies in patients with different pathological conditions focusing CCM — Scientific Report 2011 — Ongoing research 2012 113 our attention on the balance between pro and antioxidant variables and their relationship with the production of NO. In addition we focused our attention on the red blood cells as important mediators of NO bioavailability. We set up a method to investigate the arginine metabolome in RBC to better highlight the role of these cells in Arg/NO metabolic pathway in healthy and pathological conditions. Oxidative stress and Arg/NO metabolic pathway in patients undergoing cardiac surgery. We have investigated oxidative stress and Arg/NO pathway in patients candidate to the three most common cardiac surgical procedures performed in adults in western countries: coronary bypass surgery (CABG), aortic valve replacement for calcific nonrheumatic aortic stenosis (AVS) and mitral valve repair for degenerative mitral insufficiency (MVS). Adult patients undergoing cardiac surgery have decreased levels of antioxidants inducing an increase of oxidative stress compared to control subjects and, in addition, they show a trend towards impaired Arg/NO pathway in respect to controls. Patients affected by mitral valve regurgitation have more pronounced perturbations of these pathways. In a principal component analysis, we obtained, combining all these factors, a bi-dimensional plot location of the four groups. As you can see in Fig 1, MVS patients are located at a greater distance from the controls than CABG and aortic patients, suggesting that patients affected by mitral valve regurgitation show more pronounced perturbations in the considered pathways. Location of the four groups (means and SEM) in the plain defined by the two first principal components derived from markers of oxidative balance and NO pathway AVS is a degenerative and progressive condition which shares some characteristics with atherosclerosis. The association between oxidative stress and aortic fibrosis was documented in animal studies; however, to date, few data are available in humans. We measured markers of oxidative and antioxidant defences and we showed an oxidative damage due to lipid peroxidation but not to protein oxidation in patients with aortic valve stenosis. Plasma dimethylarginines and chronic kidney disease in long-term outcome of non-ST elevation acute coronary syndromes. The mechanisms linking chronic kidney disease (CKD) to adverse outcomes in patients with acute coronary syndromes (ACS), are not fully understood. Among potential key players, reduced nitric oxide (NO) synthesis due to its endogenous inhibitors, asymmetric dimethylarginine (ADMA) and symmetric dimethylarginine (SDMA) might be involved. In this study, we measured the concentrations of metabolites implicated in the NO biosynthetic pathway (arginine, ADMA, SDMA in plasma) in relation with renal function and longterm outcome in patients with ACS. Plasma arginine and ADMA were similar in patients with or without ACS whereas SDMA was higher in CKD patients. In ACS patients, SDMA increases and is associated with poor long-term outcome (the hazard ratio for adverse cardiac events was 2.95, whereas that of CKD was 1.33) . An impaired NO synthesis, as suggested by high SDMA levels, may account for the adverse prognosis of ACS patients with CKD. The Kaplam-Meier curves according to median SDMA value. 100% SDMA<=0.46µm SDMA>0.46µm 90% CABG Controls Aortic Mitral % event free patients Second principal component 80% 70% 60% 50% 40% 30% 20% 10% 0% 0 First principal component 114 CCM — Scientific Report 2011 — Ongoing research 2012 10 20 30 40 50 60 70 80 Months CCM — Scientific Report 2011 — Ongoing research 2012 115 Metabolomic evaluation of NO production in human erythrocytes: an LC-MS/MS method to assess arginine and its metabolites. Experimental studies suggest that red blood cells are involved in nitric oxide (NO) synthesis and delivery. Erythrocytes act as producers, scavengers and vehicles of NO affecting several physiological processes. NO bioavailability is linked not only to arginine and its metabolic products, ornithine and citrulline, but also to methylarginines which are inhibitors of NO synthesis. Existing methods do not allow a systematic evaluation of the metabolic and biosynthetic pathway of NO in RBC. A metabolomic approach, considering a larger number of compounds involved in NO metabolic pathway, might be helpful to understand the role of red blood cells in physiological and pathological conditions. We set up an HPLC-electrospray ionization-tandem mass spectrometry method to simultaneously detect and quantify arginine targeted metabolome, i.e. arginine, symmetric and asymmetric dimethylarginine, monomethylarginine, ornithine, citrulline. Our validated LC-MS/MS method might be useful to clarify the role of RBCs in the synthesis of NO and will be helpful for studies assessing the involvement of these cells in the regulation of blood flow under physiologic or pathological conditions. Moreover, a simple sample processing without the derivatization step suggests that this method might represent a valuable tool for diagnostic evaluation of arginine metabolome in red blood cells, making it applicable in clinical chemistry. in response to growth factors, cytokines and chemokines, they differentiate into macrophages by growing in size and increasing their lysosomal compartment, hydrolytic enzymes, mitochondria and energy metabolism. The process of differentiation results in a heterogeneous population of macrophages: they exhibit marked phenotypic differences and functional diversity as a result of a differentiation program that is subjected to environmental imprinting. Primary tissue macrophages cannot be readily expanded ex vivo and monocytic cell lines exposed to various agents that promote differentiation, are commonly used. However cell lines may not adequately address the important issue of monocyte heterogeneity and the presence of lymphocyte playing a pivotal role in macrophage differentiation and maturation. In addition, different treatments may impact on gene transcription. Although the use of cell lines is advantageous in term of availability, data cannot be easily Human macrophages obtained by spontaneous differentiation in the presence of autologous serum. extrapolated to differentiated tissue macrophages. In our laboratory we developed a model of human macrophages generated by spontaneous differentiation of adherent monocytes in the presence of autologous serum for 7 days. Mature macrophages show an increase in cytoplasmic volume and organelles compared to monocytes. Macrophages exhibit marked heterogeneity and the analysis of the morphology shows distinct subpopulations that may play distinct roles. Two different subsets are mainly identified: spindle/elongated and round cells. The characterization of the two subpopulations in terms of morphology, cytoskeletal architecture, lipid content, phagocytosis/efferocytosis and antigen expression may be important to understand the implication of macrophage heterogeneity in atherosclerosis and in other diseases. Publications Cavalca V, Colli S, Veglia F, Eligini S, Zingaro L, Squellerio I, Rondello N, Cighetti G, Tremoli E, Sisillo E. The anesthetic propofol enhances plasma tocopherol levels in patients undergoing cardiac surgery. Anesthesiology 2008;108(6):988-997 Cavalca V, Veglia F, Squellerio I, Marenzi G, Minardi F, De Metrio M, Cighetti G, Boccotti L, Ravagnani P, Tremoli E. Glutathione, vitamin E and oxidative stress in coronary artery disease: relevance of age and gender. Eur J Clin Invest 2009;39(4):267-272 Veglia F, Cavalca V, Tremoli E. OXY-SCORE: a global index to improve evaluation of oxidative stress by combining pro- and antioxidant markers. Methods in Molecular Biology 2010;594:197-213 Squellerio I, Tremoli E, Cavalca V. Quantification of arginine and its metabolites in human erythrocytes using liquid chromatography-tandem mass spectrometry. Anal Biochem 2011;412:108-110 Di Minno MN, Pezzullo S, Palmieri V, Coppola A, D’Angelo A, Sampietro F, Cavalca V, Tremoli E, Di Minno G. Genotypeindependent in vivo oxidative stress following a methionine loading test: maximal platelet activation in subjects with early-onset thrombosis. Thromb Res 2011;128(4):e43-48 A cell culture system to study macrophage differentiation and heterogeneity. Monocytes and macrophages originate from multipotent progenitor cells in bone marrow and play a pivotal role in host defense to pathogens, wound healing, angiogenesis, and various types of chronic inflammation such as atherosclerosis. Under normal conditions, monocytes migrate randomly to various tissues where they differentiate into macrophages. The external signals that control differentiation of peripheral blood monocytes are incompletely defined, however once they reach a tissue 116 CCM — Scientific Report 2011 — Ongoing research 2012 CCM — Scientific Report 2011 — Ongoing research 2012 117 4. Unit of Experimental Thrombosis and Imaging in vivo Luigi Sironi, Ph.D Head of the Unit STAFF Silvia Barbieri, Ph.D Francesca Colazzo, Ph.D Eva Tarantino, MSc Activities 2011. The Unit is located in the Department of Pharmacological and Biomolecular Sciences of the University of Milano and is dedicated to the study of vascular, cerebro- and cardiovascular diseases. These studies are carried out with a multidisciplinary approach, taking advantage of the strict collaboration among biologists, physicists and engineers. The Unit has at its disposal a remarkable combination of different imaging modalities together with a high variety of different animal models, including knock-outs, knock-ins and transgenic mice. All the animals are kept and treated according to the European rules on ethical conduct in the care and use of animals. Research program focuses on pharmacological control of brain ischemia, inflammatory diseases, neurodegenerative processes, and renal failure. Recently, the field of interest has been extended to vascular thrombosis, heart failure and myocardial ischemia and their therapeutical treatment. Moreover, the pathogenesis of thrombotic disorders, particularly regarding the role of plasmatic, vascular and cellular mediators of thrombogenesis, is also investigated as well as the molecular and cellular mechanisms involved in the thrombus generation and progression. The Unit owns an experimental scanner for magnetic resonance imaging (MRI) analysis, a Bruker Avance II operating at 4.7 T equipped with a super wide bore and a micro-imaging device that provides gradients of 14 gauss/ cm. With two specific birdcage coils (6 cm and 3.8 cm diameter) and a gas anaesthesia system, this equipment is well suited to carry out studies in mice and rats and allows to acquire “state of the art” diffusion tensor images with fast imaging methods as well as to carry out protocols for the detection of iron-oxide and gadolinium contrast agents. This equipment has been recently upgraded with a retrospective gating (IntraGate) for MRIanalysis of moving organs -in particular cardiac MRI. 118 CCM — Scientific Report 2011 — Ongoing research 2012 A VisualSonics Vevo2100 imaging platform for echographic in vivo imaging and a Millar’s MPVS Ultra system for the evaluation of cardiac parameters in beating hearts are also available. In addition, the Unit is equipped for biochemical, histological and molecular analyses of ex-vivo tissues. Main topics: 1. Use and development of MRI techniques in a multidisciplinary approach in order to visualize and follow a wide range of in vivo pathologies (epilepsy, brain and heart ischemia, neuropathy, spinal cord injury, renal diseases, heart failure). Studies are also carried out in order to follow by MRI tissue damage evolution. 2.MRI visualization of white matter organization in animals with neurodegenerative diseases taking advantage of fractional anisotropy (FA) and fiber tracking (FT) MRI techniques. 3.Evaluation, by MRI scanning, of engineered magnetic nanoparticles (MNPs) as contrast agents for the in vivo visualization of inflammatory cells. 4.Echocardiographic studies of left atrium (LA) in adult mice and evaluation of the relationship between atrium and ventricle function in acute cardiovascular conditions and in response to drug CCM — Scientific Report 2011 — Ongoing research 2012 119 Program for the Control of Global Cardiovascular Risk (3 Units) Elena TREMOLI, Ph.D Director Alessandro PAROLARI, MD, Ph.D Deputy Director Head of the Clinical Research Unit treatments, using also combined MRI and Echo approaches. 5.Understanding the cellular and molecular mechanisms involved in thrombus formation caused by different risk factors (e.g. cigarette smoke, hyperlipemia etc. ) using genetically modified animals. 6.Understanding the molecular and cellular mechanisms involved in vessel wall protection using genetically modified animals. 7.Identification and validation of new potential biomarkers of thrombosis in normal and genetically modified mice. Publications Gelosa P, Banfi C, Gianella A, Brioschi M, Pignieri A, Nobili E, Castiglioni L, Cimino M, Tremoli E, Sironi L. PPAR-alpha agonism prevents the oxidative stress and inflammatory processes involved in brain and renal damage in stroke-prone rats. J Pharmacol Exp Ther. 2010; 335:324-331 Gelosa P, Sevin G, Pignieri A, Budelli S, Castiglioni L, Blanc-Guillemaud V, Lerond L, Tremoli E, Sironi L. Terutroban, a thromboxane/prostaglandin endoperoxide receptor antagonist, prevents hypertensive vascular 120 CCM — Scientific Report 2011 — Ongoing research 2012 hypertrophy and fibrosis. Am J Physiol Heart Circ Physiol. 2011;300:H762-H768 Franzosi M, Guerrini U, Castiglioni L, Sironi L, Nobili E, Tremoli E, Caiani EG. Feasibility of quantitative analysis of regional left ventricular function in the post-infarct mouse by magnetic resonance imaging with retrospective gating. Comput Biol Med. 2011;41:829-37 Barbieri SS, Ruggiero L, Tremoli E, Weksler BB. Suppressing PTEN activity by tobacco smoke plus interleukin-1beta modulates dissociation of VE-cadherin/ beta-catenin complexes in endothelium. Arterioscler Thromb Vasc Biol. 2008;28:732-738 Barbieri SS, Zacchi E, Amadio P, Gianellini S, Mussoni L, Weksler BB, Tremoli E. Cytokines present in smokers’ serum interact with smoke component to enhance endothelial dysfunction. Cardiovasc Res. 2011; 90:475-483 Barbieri SS, Amadio P, Gianellini S, Zacchi E, Weksler BB, Tremoli E. Tobacco smoke regulates the expression and activity of microsomal-prostaglandin E synthase-1: role of prostacyclin and NADPH-oxidase. FASEB J. 2011 [Epub ahead of print] 1. José Pablo WERBA, MD Head of the Unit of Atherosclerosis Prevention 2. Damiano BALDASSARRE, Ph.D Head of the Unit of Arterial Morphology and Function 3. Fabrizio VEGLIA, Ph.D Head of the Unit of Biostatistics Cardiovascular diseases represent the number one killer in developed countries. Scientific evidences demonstrate the efficacy and cost/effectiveness of specific vascular screening procedures, lifestyle changes and drug treatments in reducing cardiovascular morbidity and mortality in patients with overt cardiovascular disease (secondary prevention) or at high relative or absolute risk (targeted primary prevention). The identification and global control of conventional and emerging risk factors is a mainstay in decreasing the incidence and rate of recurrence of cardiovascular events. These activities are carried out by integrating patient care and focused clinical research. The cultural principle shared by all the members of the team is: “make rational use of consolidated evidencebased early diagnostic tools and effective therapies, and foster translational research aimed at improving individual risk assessment and global risk reduction”. CCM — Scientific Report 2011 — Ongoing research 2012 121 1. Unit of Atherosclerosis Prevention José Pablo WERBA, MD Head of the Unit STAFF Costanza Boiti, MD Monica Giroli, Biologist Nutritionist, Ph.D Federica Laguzzi, MSc 122 CCM — Scientific Report 2011 — Ongoing research 2012 The Unit of Atherosclerosis Prevention provides long-term clinical care and is run by specialists in internal medicine, nutritionists and research fellows. A specialized approach to prevention has demonstrated its efficacy in improving not only the control of risk factor but also patient prognosis in different centers both in the United States and in Europe. So far, about 2900 patients were included in the program, most of them in secondary or high risk primary prevention, the later primarily focused on first degree relatives of probands with overt disease. In tight link with patient care, the Unit carries out original research initiatives aimed to uncover the many yet-unidentified environmental or genetic determinants of: 1) cardiovascular risk, 2) earliness of vascular event presentation, 3) plaques distribution within the arterial tree, 4) type of clinical presentation and 5) event recurrence. In addition, the Unit collaborates in studies aimed to investigate the pathophysiology of heart-harmful diseases (e.g. obesity, diabetes, liver steatosis, very high or very low HDL cholesterol levels) as well as mechanisms of efficacy/ resistance, pleiotropic and side effects of consolidated and novel drugs for the control of cardiovascular risk. Dietary factors also play a fundamental role in cardiovascular disease and its prevention. Our research activities in this field focus on the search of an optimal diet and potential nutrient-drug interactions. Biological samples are systematically collected from patients to create a plasma and DNA bank. The availability of a clinical database and a biobank is extremely useful for observational studies of associations between genotype and clinical phenotype and for selection of patients to be included in experimental studies of pharmacogenetics and pharmacogenomic aimed to test the efficacy and tolerability of drugs in different fields such as thrombosis, diabetes, hyperlipidemia, hypertension, and others. Information and biological samples collected are safely stored to test new hypothesis that could emerge along with upcoming scientific knowledge. Publications Baldassarre D, Castelnuovo S, Frigerio B, Amato M, Werba JP, De Jong A, Ravani AL, Tremoli E, Sirtori CR. Effects of timing and extent of smoking, type of cigarettes, and concomitant risk factors on the association between smoking and subclinical atherosclerosis. Stroke. 2009;40(6):1991-8 Baldassarre D, Werba JP, Castelnuovo S, Frigerio B, Amato M, Ravani A, Veglia F, Sirtori CR and Tremoli E. The metabolic syndrome predicts carotid intima-media thickness no better than the sum of individual risk factors in a lipid clinic population. Atherosclerosis. 2010;210:214-9 Simiele F, Recchiuti A, Mattoscio D, De Luca A, Cianci E, Franchi S, Gatta V, Parolari A, Werba JP, Camera M, Favaloro B, Romano M.Transcriptional regulation of the human FPR2/ALX gene: evidence of a heritable genetic variant that impairs promoter activity. FASEB J. 2012;26(3):1323-33 Misaka S, Kawabe K, Onoue S, Werba JP, Giroli M, Kimura J, Watanabe H, Yamada S. Development of rapid and simultaneous quantitative method for green tea catechins on the bioanalytical study using UPLC/ESI-MS. Biomed Chromatogr. 2012 [Epub ahead of print] CCM — Scientific Report 2011 — Ongoing research 2012 123 2. Unit of Arterial Morphology and Function Damiano BALDASSARRE, Ph.D Head of the Unit STAFF Mauro Amato, Ph.D Beatrice Frigerio, Ph.D student Alessio Ravani, MSc Daniela Sansaro, MSc The Unit of Arterial Morphology and Function is focused on the non-invasive assessment of early atherosclerosis. Most studies are performed using B-mode ultrasound, which provides information on the presence and extent of atherosclerotic plaques, arterial wall thickness (intima-media thickness or IMT) and vessel lumen diameter of superficial arteries. These variables are used as “surrogate” markers of atherosclerosis. The experience of the group, which was the first to describe carotid IMT (C-IMT) in 1986, is internationally recognized. The relevance ascribed to C-IMT by the scientific community is evidenced by the ever-growing number of studies which use this ultrasonic variable. Besides, changes in C-IMT are the only marker of preclinical atherosclerosis accepted by the American Heart Association, in place of hard clinical endpoints, in pharmacological studies for the 124 CCM — Scientific Report 2011 — Ongoing research 2012 approval of new drugs. In 2008 the Unit was involved in an International committee whose mission was to develop Guidelines to transfer the scientific C-IMT knowledge into clinical practice. This objective was driven also by findings of our group, showing that C-IMT may improve the power of vascular risk factors to predict new vascular events in the large number of patients who, according to available risk algorithms, fall into an intermediate risk category. In this regard, the Unit is strongly committed in developing new strategies for the better estimation of overall cardiovascular risk based on the concept of “integrated biomarkers”. By measuring acute changes induced by flow in the diameter of the brachial artery (flow-mediated vasodilatation or FMD), B-Mode ultrasound may also provide information about endothelial function. Patients exposed to risk factors show endothelial dysfunction even in the absence of overt atherosclerotic disease. Indeed, endothelial dysfunction is a very early index and predictor of atherosclerotic disease. Main research topics of the Unit are: • Identification of new atherosclerosis risk factors on the basis of their effect on C-IMT and endothelial function. • Improvement of new tools for the study of atherosclerosis and for improving predictability of vascular events. • Assessment of the association between C-IMT progression, conventional and emerging risk factors and incidence of cardiovascular events. • Assessment of the effects of pharmacological treatments on morphological and functional properties of superficial arteries. In addition, the Unit coordinates and acts as core laboratory in national and international multicentre studies on the epidemiology of atherosclerosis. Publications Baldassarre D, Castelnuovo S, Frigerio B, Amato M, Werba JP, De Jong A, Ravani AL, Tremoli E, Sirtori CR. Effects of timing and extent of smoking, type of cigarettes and concomitant risk factors on the association between smoking and subclinical atherosclerosis. Stroke. 2009;40(6):1991-8 intima-media thickness in a European population: the IMPROVE study. Eur Heart J. 2010;31(5):614-22 Calabresi L, Baldassarre D, Castelnuovo S, Conca P, Bocchi L, Candini C, Frigerio B, Amato M, Arca M, Boscutti G, Cattin L, Gesualdo L, Sampietro T, Vaudo G, Veglia F, Calandra S, Franceschini G. Functional LCAT is not required for efficient atheroprotection in humans. Circulation. 2009;120(7):628-35 Baldassarre D, Werba JP, Castelnuovo S, Frigerio B, Amato M, Ravani A, Veglia F, Sirtori CR, Tremoli E. The metabolic syndrome predicts carotid intima-media thickness no better than the sum of individual risk factors. Atherosclerosis. 2010;210(1):214-9 Baldassarre D, Nyyssönen K, Rauramaa R, de Faire U, Hamsten A, Smit AJ, Mannarino E, Humphries SE, Giral P, Grossi E, Veglia F, Paoletti R, Tremoli E, on behalf of the IMPROVE study group. Cross-sectional analysis of baseline data to identify the major determinants of carotid Interleukin-6 Receptor Mendelian Randomisation Analysis (IL6R MR) Consortium, A.D. Hingorani, J.P.Casas. The interleukin-6 receptor as a target for prevention of coronary heart disease: a mendelian randomisation analysis. Lancet 2012;379(9822):1214-24 CCM — Scientific Report 2011 — Ongoing research 2012 125 3. Unit of Biostatistics Fabrizio VEGLIA, Ph.D Head of the Unit STAFF Francesca Bovis, MSc Calogero C. Tedesco, MSc The Unit of Biostatistics provides advice, support and implementation in protocol design, quality control of databases, data coding, input, and statistical analysis of clinical studies performed by the clinical teams of Centro Cardiologico Monzino. It collaborates in the design, and is in charge of data analyses, of epidemiological, clinical and experimental studies performed by the research Units. It acts as reference data management and data analyses centre in international epidemiological studies. In addition, the Unit performs autonomous research activities on a wide range of topics, focusing on epidemiology of cardiovascular diseases and statistical methodology as follows: • Epidemiology of subclinical atherosclerosis: links with social class, geography and diet • Development of innovative methods for the analysis of complex ultrasound measures • Development of summary scores based on clusters of soluble markers of inflammation, oxidative balance and endothelial function • New models for the analysis of familial aggregation of atherosclerosis • Development of theoretical models of atherosclerosis progression • Development of new methods to assess carotid IMT progression • Improvement of statistical approaches aimed to optimize algorithms for risk prediction. Publications Montorsi P, Caputi L, Galli S, Ciceri E, Ballerini G, Agrifoglio M, Ravagnani P, Trabattoni D, Pontone G, Fabbiocchi F, Loaldi A, Parati E, Andreini D, Veglia F, Bartorelli AL. Microembolization during carotid artery stenting in patients with high-risk, lipid-rich plaque. A randomized trial of proximal versus distal cerebral protection. J Am Coll Cardiol. 2011;58(16):1656-63 Pontone G, Andreini D, Bartorelli AL, Bertella E, Mushtaq S, Annoni A, Formenti A, Chiappa L, Cortinovis S, 126 CCM — Scientific Report 2011 — Ongoing research 2012 Baggiano A, Conte E, Bovis F, Veglia F, Foti C, Ballerini G, Fiorentini C, Pepi M. Radiation dose and diagnostic accuracy of multidetector computed tomography for the detection of significant coronary artery stenoses A metaanalysis. Int J Cardiol. 2011 [Epub ahead of print] Di Carlo A, Lamassa M, Wellwood I, Bovis F, Baldereschi M, Nencini P, Poggesi A, Cramaro A, Pescini F, Lucente G, Wolfe C A, Inzitari D,European Registers Stroke EROS Project. Stroke unit care in clinical practice: an observational study in the Florence center of the European Registers of Stroke (EROS) . Eur J Neurol 2011; 18(5):686-94 Calabresi L, Baldassarre D, Simonelli S, Gomaraschi M, Amato M, Castelnuovo S, Frigerio B, Ravani A, Sansaro D, Kauhanen J, Rauramaa R, de Faire U, Hamsten A, Smit AJ, Mannarino E, Humphries SE, Giral P, Veglia F, Sirtori CR, Franceschini G, Tremoli E. Plasma lecithin:cholesterol acyltransferase and carotid intima-media thickness in European individuals at high cardiovascular risk. J Lipid Res. 2011;52(8):1569-74 Parolari A, Tremoli E, Cavallotti L, Trezzi M, Kassem S, Loardi C, Veglia F, Ferrari G, Pacini D, Alamanni F. Do statins improve outcomes and delay the progression of nonrheumatic calcific aortic stenosis? Heart. 2011; 97(7):523-9. CCM — Scientific Report 2011 — Ongoing research 2012 127 Laboratory of Immunology and Functional Genomics Gualtiero COLOMBO, MD Director STAFF Federica Saporiti, Ph.D Paolo Kunderfranco, Ph.D Giuliano Stirparo, Ph.D student Luca Piacentini, MSc Elisa Bono, Technician 128 CCM — Scientific Report 2011 — Ongoing research 2012 The Laboratory of Immunology and Functional Genomics was established in September 2010. The Lab work is focused on the following research fields: (1) antiinflammatory pathways in the pathophysiology of atherothrombosis; (2) immune-mediated mechanisms that contribute to the formation of atherosclerotic plaques and the occurrence of cardiovascular events; (3) genomic approaches (such as transcriptome or targeted genome resequencing projects) to uncover potentially useful biomarkers and to disentangle gene functions and interactions in atherosclerosis and cardiovascular diseases (CVDs); (4) genetics of CVDs. Functional genomics includes assessment of functionrelated aspects of the genome itself, such as analysis of mutations that cause function loss or alteration, as well as measurements of molecular activities and investigations on dynamic aspects, such as gene transcription and translation and their control. The latter comprise a number of “-omics” such as transcriptomics (gene expression, microRNA and non coding RNA profiling), proteomics (protein expression), phosphoproteomics and metabolomics. Together these measurement modalities quantify the various biological processes and power the understanding of gene and protein functions and interactions. The ultimate goal of the Laboratory is to identify molecular biomarkers and/or clarify pathogenic mechanisms that would help design therapeutic strategies to prevent and/or reverse atherosclerosis progression and/or cardiovascular events. To achieve these objectives, the group components have a solid technical experience in molecular and cell culture techniques, as well as developed skills in analysis of complex biological systems. The group focuses on the analysis and mining of microarray data (genotyping, gene expression, and microRNA profiling), proteomic profiles (antibody arrays), and deep sequencing data (transcriptome, epigenetic modifications, and targeted resequencing). Using modern bioinformatics tools, network-based analysis are performed relying upon databases that integrate clinical, imaging, molecular, and genomic data, in a systematic examination of the pathophysiological bases of atherothrombosis and related pathological conditions. The Lab work is also in support for genomics studies in collaboration with other research groups of the CCM. Immunology and atherosclerosis: relevance in CVDs Atherosclerosis is a complex chronic inflammatory disease that affects large- and medium-size arteries and induces alterations of the phenotypes of vascular cells. All phases of atherosclerosis are regulated by inflammatory mechanisms that provide overlapping networks of pathways involved in the regulation of immune cell functions, activation of endothelium, and alteration of metabolic parameters. Increasing evidence suggests that components of the immune system may alter lipid metabolism and thus affect atherosclerosis. Central in this field is the characterization of aberrant responses of macrophages, B and T lymphocytes, platelets, and vascular smooth muscle cells. Most common forms of CVDs are believed to be multifactorial and to result from interaction of many genes, each with a relatively small effect, working alone or in combination with modifier genes and/ CCM — Scientific Report 2011 — Ongoing research 2012 129 or environmental factors. The identification and the characterization of these genes and their modifiers would enhance prediction of cardiovascular risk. Knowledge about when, where, and to what extent a gene is expressed is critical for understanding the activity and biological roles of the protein product of the gene in relation to CVDs. Understanding the role of these genes on inflammation and the immune system is of great importance. All these data will help to identify potential therapeutic targets for the prevention and treatment of atherosclerosis and other CVDs. Emerging technologies for functional genomics Functional genomics apply genomic information by investigating large sets of molecules (DNA, RNA, proteins) in numerous samples of different origins (extracts, cells, tissues) using a widening range of tools, including advanced array technologies and nextgeneration sequencing. The Lab has been equipped with a set of devices for multiple purposes. DNA arrays are used for genotyping and expression analysis. Genotyping technologies enable whole genome association studies for complex disease gene mapping. Several million common SNPs are known for the human genome, potentially allowing inheritance to be traced for factors that predispose to common conditions. Transcriptome analysis, monitoring the activity of a genome by measuring mRNA expression levels, provides important biological insights. Recent clinical studies of CVDs demonstrate that expression analysis of large gene sets can identify molecular profiles correlated with disease states, which may then be developed as diagnostic tools. Antibody arrays are used for protein expression studies and as discovery tools in autoimmunity. Whole proteome chips allow high throughput array-based characterization of functional protein interactions. Gene functions can be revealed by loss of function assays. Gene knockdown by modulation of mRNA 130 CCM — Scientific Report 2011 — Ongoing research 2012 turnover using RNA interference (RNAi) has become the favorite method for inhibiting expression of targeted genes. RNAi has been combined with cell microarray systems for screening, allowing analysis of the impact of thousands of genes on many cell biological functions in a single experiment. Finally, a new generation of sequencing technologies has provided unprecedented opportunities for high throughput functional genomic research. To date, these technologies have been applied in a variety of contexts, including whole genome sequencing, targeted resequencing, detection of transcription factor binding sites by chromatin immunoprecipitation sequencing, methylation analysis, gene expression profiling, and non-coding RNA discovery and profiling. A typical application is searching genomes and/or transcriptomes for alterations that could explain individual phenotypic variation, particularly disease. Another key area that takes advantage from this technique is epigenetics, which combines genetics and environment to address genome plasticity and the control of gene expression by, for instance, differential DNA methylation and histone modification. Bioinformatics & systems biology In the present era of post-genome research, the various high throughput -omics approaches allow to think in terms of construction of conceptual models of the living cell. This global and inter-disciplinary approach, designated “systems biology”, requires the organization and integration of complex experimental knowledge and its expression in models with sufficient predictive capacity. Systems biology aims to analyze the relationships among the elements in a system in response to genetic or environmental perturbations, where a biological system may encompass molecules, cells, organs, or individuals. Systems biology acts as a natural link between experimental functional genomics activities and computational biology and bioinformatics. Relevant computational steps are the organization of complex genomics information, modeling of the biological system, prediction of properties of uncharacterized systems components, and the generation of hypotheses concerning the reaction of the system to external perturbation. The computational aspects of systems biology require a combination of classical developments in bioinformatics, followed by the application of mathematical modeling tools. This unique combination of expertise is inherently multidisciplinary and requires input from biomedical experimental research, high throughput technologies, life science image processing, bioinformatics, and mathematics. This is the biggest challenge to face for the Lab for the next future. Colombo G, Sordi A, Lonati C, Carlin A, Turcatti F, Leonardi P, Gatti S, Catania A. Treatment with a-Melanocyte Stimulating Hormone preserves calciumhandling proteins in rat heart allografts. Brain Behav Immun 2008; 22:817-23 Functional genomics & biomedicine The technological advances in genotyping, expression profiling, coupled with systems biology, offer exciting and promising advances in cardiovascular medicine, both in understanding the basis of CVDs and in improved diagnosis and therapy. The combination of -omics information will allow early and more accurate diagnosis of disease and/or prediction of disease onset and progression. In addition, the redefinition of disease subtypes through functional genomics is likely to provide insight of differential response to therapy: understanding individual responses to drugs will have implications for their use and development. Colombo G, Gertow K, Marenzi G, Brambilla M, De Metrio M, Tremoli E, Camera M. Gene expression profiling reveals multiple differences in platelets from patients with Stable Angina or non-ST elevation Acute Coronary Syndrome. Thromb Res 2011; 128:161-8 Achilli F, Malafronte C, Lenatti L, Gentile F, Dadone V, Gibelli G, Maggiolini S, Squadroni L, Di Leo C, Burba I, Pesce M, Mircoli L, Capogrossi MC, Di Lelio A, Camisasca P, Morabito A, Colombo G, Pompilio G. Granulocyte Colony-Stimulating Factor attenuates left ventricular remodelling after acute anterior STEMI: results of the single-blind, randomized, placebo-controlled multicenter stem cell mobilization in Acute Myocardial Infarction (STEM-AMI) trial. Eur J Heart Fail 2010; 12:1111-21 Burba I, Colombo GI, Staszewsky LI, De Simone M, Devanna P, Nanni S, Avitabile D, Molla F, Cosentino S, Russo I, De Angelis N, Soldo A, Biondi A, Gambini E, Gaetano C, Farsetti A, Pompilio G, Latini R, Capogrossi MC, Pesce M. Histone deacetylase inhibition enhances self renewal and cardioprotection by human cord bloodderived CD34+ cells. PLoS One 2011; 6:e22158 Publications Cortelezzi A, Colombo G, Pellegrini C, Silvestris I, Moronetti Mazzeo L, Bosari S, Lambertenghi Deliliers G, Fracchiolla NS. Bone marrow glycophorin-positive erythroid cells of myelodysplastic patients responding to high-dose rHuEPO therapy have a different gene expression pattern from those of non-responders. Am J Hematol 2008; 83:531-9 CCM — Scientific Report 2011 — Ongoing research 2012 131 Laboratory of Vascular Biology and Regenerative Medicine Maurizio CAPOGROSSI, MD Director Giulio POMPILIO, MD, Ph.D Deputy Director Head of the Clinical Research Unit STAFF Daniele Avitabile, Ph.D Ilaria Burba, Ph.D Chiara Cencioni, Ph.D Yuri D’Alessandra, Ph.D Elisa Gambini, Ph.D Giuseppina Milano, Ph.D Patrizia Nigro, Ph.D Ombretta Pozzoli, Ph.D Angela Raucci, Ph.D Alessandra Rossini, Ph.D Francesco Spallotta, Ph.D Lorena Verduci, Ph.D Valerio Azzimato, Ph.D student Marco De Simone, Ph.D student Viviana Meraviglia, Ph.D student Matteo Vecellio, Ph.D student Serena Balasso, MSc Beatrice Bassetti, MSc Maria Cristina Carena, MSc Alessandro Scopece, MSc Paolo Devanna, BSc Consultant: Carlo Gaetano, MD 132 CCM — Scientific Report 2011 — Ongoing research 2012 The Laboratory of Vascular Biology and Regenerative Medicine and the Clinical Research Unit of Cardiovascular Regeneration work in synergy to develop strategies for the treatment of cardiac and peripheral vascular diseases. Basic molecular studies and experiments in animal models of cardiac and hindlimb ischemia are complementary to the translation of cell therapy interventions to patients. microRNAs in cardiovascular diseases microRNAs in coronary artery syndromes. microRNAs (miRNAs) are small non-coding RNAs that regulate translation of mRNAs into proteins. Dysregulation in the expression of cardiac miRNAs has been associated with myocardial infarction and other forms of heart disease. Recently, miRNAs have been identified in the bloodstream and we have found marked changes in the plasma levels of some circulating miRNAs in patients and experimental animals with acute myocardial infarction. These observations raise the possibility that some miRNAs may be sensitive biomarkers of cardiac damage and that they may also have biological effects on some cell functions. Ongoing studies are aimed at establishing circulating miRNAs sensitivity and specificity as biomarkers of coronary artery syndromes and of MI in patients with borderline troponin elevation. microRNAs in oxidative stress. A variety of clinically relevant conditions including tissue damage in response to ischemia/reperfusion, diabetes, anti-cancer therapy with anthracyclines and aging are associated with enhanced oxidative stress. We have found that miR-200 family is markedly up-regulated upon cell exposure to oxidative stress and plays a pivotal role in cell cycle inhibition, senescence and death. Cardiovascular epigenetics Epigenetics and cell reprogramming. Epigenetic mechanisms modulate lineage-decisions in uncommitted cells; primitive stem cells have hyperacetylated histones that become progressively deacetylated during their commitment. Our laboratory focuses on the epigenetic mechanisms that induce mesenchymal cell to acquire a phenotype closer to that of myocardial and vascular precursors and on drugs that act on chromatin structure, including histone deacetylase inhibitor and acetylases inhibitors/activators, and may confer enhanced plasticity and therapeutic potential to cells for cardiovascular transplantation. Specifically, we are currently testing different combination of epigenetically active molecules aimed at generating functionally competent cardiovascular precursor from adult cardiac cells Epigenetics of metabolic memory. Diabetes is a condition in which all organs are exposed to high glucose for a prolonged period of time and a generalized functional impairment may occur as a consequence of the hyperglycemia. Recent observations revealed that, even after normalization of glycemia by insulin treatment of other pharmacological interventions, the functional CCM — Scientific Report 2011 — Ongoing research 2012 133 impairment often remains unchanged. Epigenetic cues are called in as the mechanistic reason of this alteration although their nature is still poorly characterized. In our laboratory we recently observed that cardiac and bone marrow-derived mesenchymal stem cells may have different growth ratio in relationship to the presence of diabetes in the donor patient. Specifically, mesenchymal cells derived from diabetic patients do not replicate as efficiently as those obtained from nondiabetic individuals. Biological and molecular analyses revealed that histones and DNA methylation may play an important role in determining this impairment. Experiments are now in progress to investigate the origin of this alteration with special attention paid to the potential role of epigenetic enzymes including histone (HMTS) and DNA (DNMTS) methylases, Lysine acetylases (HATS) and deacetylases (HDACS) protein families. Cardiovascular regeneration Zebrafish as a model system for regenerative medicine. Zebrafish (Danio rerio) is capable of complete cardiac regeneration after partial ventricular resection and is emerging as an excellent model for in vivo studies in regenerative medicine. Our studies using this model focus on the molecular mechanisms underlying the regenerative cardiac response induced by hypoxia/ reoxygenation injury and on studies of stem cell plasticity following their transplant in zebrafish. HMGB1 and cardiac regeneration. High-mobility group box 1 protein (HMGB1) is a chromatin protein that is released by inflammatory and necrotic cells. Extracellular HMGB1 signals tissue damage and modulates stem cell function. We demonstrated that local delivery of HMGB1 in the mouse heart, acutely after infarction, induces a regenerative response by activating resident cardiac stem cells in conjunction with Notch/Wnt11 signalling pathways activation. Further, we found that HMGB1 improves left ventricular remodelling following myocardial infarction and markedly enhances miR-206 expression 134 CCM — Scientific Report 2011 — Ongoing research 2012 in the heart; this effect was associated with diminished collagen content in the left ventricle, increased matrix metalloprotease (MMP) – 2 and -9 activity, and miR-206mediated down-regulation of TIMP-3. Epicardial cells. During development, the epicardium is a source of multipotent cells which give rise to coronary vessels and cardiomyocytes. We have shown that the adult epicardium contains a stem cell population which can give origin to myocardial and vascular cells; these cells are activated following acute myocardial infarction and contribute to the regenerative response triggered by acute ischemia and necrosis. Further, we have shown that epicardial cells fuse with skeletal myotubes with high efficiency and differentiate toward the skeletal muscle phenotype. Human cardiac cells for heart regeneration. The heart contains resident stem cells that maintain homeostasis by replacing lost myocytes. In our laboratory we perform studies both with human cardiac c-kit+ cells (CPCs) and Cardiac Stromal Cells (CStCs). Human cardiac c-kit+ cells. We are correlating the clinical profile of patients undergoing cardiac surgery with biological features of CPCs obtained from right atrium surgical specimens. Our preliminary results show that a number of variables associated with patient’s demographic, cardiologic status and medications have a different impact on resident CPCs number and function. These results may provide new insights for the understanding of cardiac homeostasis. Human cardiac stromal cells. We have identified a population of human cardiac stromal cells with mesenchyma-like features (CStCs) which we have compared to bone marrow stromal cells (BMMSC) from the same patient. Although CMSC and BMMSC share common mesenchymal markers, CstCs are more competent than BMMSC in differentiating toward the myocardial and vascular lineages, both in vitro and in vivo. In addition, when injected into the heart in a rat model of post-myocardial infarction heart failure, CMSC differentiated into cardiomyocytes and improved cardiac function more efficiently than BMMSC. Therefore, CStCs appear as a potentially useful cell type for tissue engineering approach. In this light, we are currently evaluating the ability of CStCs to efficiently repopulate decellularized aortic valve homografts potentially useful for clinical applications. In addition, we are presently comparing CStC ability to differentiate into cardiovascular cell types with that of cells isolated from a developmentally younger tissue, i.e. chorionic villus stroma-derived cells. Cardio-oncology. Cardiac toxicity is one of the most devastating sequelae of cancer therapy with anthracyclines and trastuzumab; it limits the possibility of further therapy, worsens patients’ quality of life and increases mortality. It is conceivable that CPCs and CStCs may be obtained from endomyocardial biopsy samples prior to initiating anticancer drugs administration; subsequently, autologous cells may be used to treat those patients who develop cardiac toxicity and heart failure. Therefore we have developed a rodent model of doxorubicin and trastuzumab cardiac toxicity in which to examine the potential therapeutic action of cardiac cell transplantation. Further, in this animal model we are also examining miR-200 family role to the response to anticancer drugs. CCM — Scientific Report 2011 — Ongoing research 2012 135 Cell enhancement strategies. Peripheral blood- or bone marrow-derived endothelial progenitor cells (EPCs) induce neo-vascularization in ischemic tissues. However, EPCs isolated from elderly patients and from individuals with cardiovascular risk factors exhibit an impaired therapeutic potential. Therefore, we characterized two different pre-conditioning strategies aimed at enhancing EPCs repair ability. We analyzed the effect of Valproic acid (VPA), an epigenetic drug with histone deacetylase inhibitory action. VPA treatment of CD34+ cells isolated from human umbilical cord blood preserves an immature subset of cells in culture and increases their self-renewal ability. Furthermore, VPA-treated human CD34+ cells improved ischemic myocardium protection in an immunodeficient mouse model of myocardial infarction. In addition, we examined the effect of bone marrow-derived ckit+ cell (BM-derived EPC) preconditioning with a brief exposure to low pH (acidic pre-conditioning; APC). APC increased CXCR4 expression and phosphorylation levels via a nitric oxide-dependent mechanism. Further, APC enhanced SDF-1-directed migration and differentiation into endothelial cells. Lastly, APC-treated ckit+ cells exhibited an improved angiogenic and regenerative potential following their transplantation in a mouse model of hindlimb ischemia. Clinical Research Unit of Cardiovascular Regeneration is involved in clinical studies of cell therapy for cardiovascular ischemic disorders, including myocardial infarction complicated by ventricular dysfunction, refractory ischemic cardiomyopathy, limb ischemia. On the base of a previous multicenter trial (STEMAMI) on ST-elevated myocardial infarction, the Unit is presently planning to coordinate a national, multicentre, randomized, placebo-controlled, Phase III trial to demonstrate that granulocyte colony-stimulating factor (G-CSF) therapy, in addition to state-of-the-art treatment, may significantly improve clinical outcome in 1530 patients with reduced left ventricular ejection fraction (≤45%) after successful reperfusion for large anterior acute myocardial infarction (STEMAMI OUTCOME). Furthermore, the Unit has consolidated the experience in treating patients with refractory myocardial ischemia using autologous, bone marrowderived CD133+ cells isolated under GMP conditions and injected directly into the myocardium, finalizing a first series of 10 patients with no-option refractory angina. Finally, the Unit has a specific interest in critical limb ischemia, on the base of previous Phase II and Phase III trials (TALISMAN and TAMARIS) of gene therapy with the growth factor FGF1. GMP standardization of CD133+ cells isolation methods for cardiovascular repair. The US Food and Drug Administration (FDA) and the European Medicines Agency (EMEA) have established regulatory frameworks to ensure high safety standards and biological quality of cell-based medicinal products (CBMPs) that must comply with good manufacturing practice (GMP) specifications. We have performed bone marrow-derived CD133+ cells isolation and release under GMP compliant procedures; these cells were used for autologous cell transplantation in patients with refractory cardiac ischemia. Publications Spallotta F, Rosati J, Straino S, Nanni S, Grasselli A, Ambrosino V, Rotili D, Valente S, Farsetti A, Mai A, Capogrossi MC, Gaetano C, Illi Barbara. Nitric oxide determines mesodermic differentiation of mouse embryonic stem cells by activating class IIa histone deacetylases: potential therapeutic implications in a mouse model of hindlimb ischemia. Stem Cells. 2010. 28(3):431-42 Regenerative therapy and its clinical application. The 136 CCM — Scientific Report 2011 — Ongoing research 2012 Achilli F, Martelli F, Maggiolini S, Marenzi G, Pompilio G, Maurizio MC. Circulating MicroRNAs are new and sensitive biomarkers of myocardial infarction. Eur Heart J. 2010. 31(22):2765-2773 Achilli F, Malafronte C, Lenatti L, Gentile F, Dadone V, Gibelli G, Maggiolini S, Squadroni L, Di Leo C, Burba I, Pesce M, Mircoli L, Capogrossi MC, Di Lelio A, Camisasca P, Morabito A, Colombo G, Pompilio G. Granulocyte colony-stimulating factor attenuates left ventricular remodelling after acute anterior stemi.Results of the single-blind, randomized, placebo-controlled multicenter stem cell mobilization in acute myocardial infarction (STEM-AMI) trial. Eur J Heart Fail. 2010. 12(10):1111-1121 Colussi C, Rosati J, Straino, Spallotta F, Berni R, Stilli D, Rossi S, Musso E, Macchi E, Mai A, Sbardella G, Castellano S, Chimenti C, Frustaci A, Nebbioso A, Altucci L, Capogrossi MC, Gaetano C. Nε-lysine Acetylation Determines Dissociation from GAP-junctions and Lateralization of Connexin 43 in Normal and Dystrophic Heart. Proc Natl Acad Sci. 2011. 108(7):2795-2800 Cencioni C, Melchionna R, Straino S, Romani M, Cappuzzello C, Annese V, Wu JC, Pompilio G, Santoni A, Gaetano C, Napolitano M, Capogrossi MC. Ex vivo acidic preconditioning enhances bone marrow ckit+ cell therapeutic potential via increased CXCR4 expression. Eur Heart J. 2011. [Epub ahead of print] D’Alessandra Y, Devanna P, Limana F, Straino S, Di Carlo A, Brambilla PG, Rubino M, Carena MC, Spazzafumo L, De Simone M, Micheli B, Biglioli P, CCM — Scientific Report 2011 — Ongoing research 2012 137 Laboratory of Cardiovascular Tissue Engineering Gianluca POLVANI, MD Director Maurizio PESCE, Ph.D Deputy Director STAFF Maria Cristina Vinci, Ph.D Rosaria Santoro, Ph.D Francesca Prandi, Ph.D student The mission of the Laboratory of Cardiovascular Tissue Engineering is to devise strategies to derive a new generation of cardiovascular implants and devices, by combining cardiovascular stem cell knowledge and material/biomechanic expertise. Starting from basic investigations on human-derived cardiovascular progenitors such as cord blood-/peripheral blood-/ bone marrow-derived endothelial progenitor cells (EPCs), cardiac resident stem cells (CSCs), saphenous vein progenitors (SVPs) and the so called aortic valve interstitial cells (VICs), the mechanism linked to physiological or pathological differentiation of these cells is being studied by applying “high content” molecular analysis and high throughput material screening methods which allow a rapid search for novel bio-materials (polymers, hydrogels and biological scaffolds) to embed stem cells in culture. In this scenario, also the investigation on strain- and mechanical stress-associated stem cells response appears particularly relevant. Histone code of human endothelial progenitor cell function and disease: from memory to risk. (Fig. 1) Bone marrow-derived endothelial progenitor cells (EPCs) play a role in physiological endothelial cell turnover through innate endothelialization capacity, and protect arteries from atherosclerosis and damage-associated stenosis. The amount and the activity of circulating EPCs are dramatically decreased with age, in patients with diabetes, and in other risk conditions associated with cardiovascular diseases (CVD). Therefore, the use of these cells for engineering blood vessels appears limited. While attempts have been made to restore innate EPCs functions 138 CCM — Scientific Report 2011 — Ongoing research 2012 through various pharmacological interventions, the molecular basis of these defects remain elusive. Recent data have highlighted the existence of an epigenetic memory, which can be established as a consequence of metabolic dysfunction and risk conditions. At the molecular level, these defects are “written” in the genome as changes in the DNA and chromatin modifications underpinning an altered gene expression. In the attempt to mimick risk conditions for potential phenotypic and functional transformation of human EPCs, we have set up an assay to expose these progenitors to oxidized LDL, a form of lipoprotein abundantly present in the atherosclerotic plaque and known to activate innate immunity associated to atherosclerosis progression. We have found that these cells are converted in functionally active antigen presenting cells, able to activate T-lymphocytes proliferation in mixed leukocyte reactions (MLR), and secrete a variety of pro-inflammatory cytokines. Molecular profiling of these cells and their epigenetic makeup in response to Ox-LDL exposure, are currently being analyzed. This research is performed by our Laboratory in collaboration with the College of Physicians and Surgeons, Columbia University, New York, USA, and the Laboratory of Functional Genomics at Centro Cardiologico Monzino. CCM — Scientific Report 2011 — Ongoing research 2012 139 Fig. 1 Fig. 2 Circulating pro-angiogenic cells (CFU-ECs) Human SVPs - Passage 1 oxidized-LDL SV CONDITIONING BIOREACTOR Antigen presenting cells (APCs) Pressure transducer Pc Patm Valve SV housing Reservoir Pump SV Human SVPs - Passage 4 Lymphocyte (➞) activation A mechano-biology approach to understand the role of saphenous vein-resident vascular progenitors (SVPs) in the establishment and progression of vein bypass graft disease. (Fig. 2) Implantation of saphenous vein (SV) segments is routinely used to generate aorto-coronary bypass grafts (CABG) to revascularize the ischemic myocardium. It is estimated that between 10 and 15 years after implantation, 50% of vein bypasses undergo functional failure (vein graft disease, VGD), due to accumulation of smooth muscle cells (SMCs) in the intima. While molecular and signaling pathways linked to smooth muscle cell activation in VGD have been widely investigated, the role of other veinintrinsic and vein-extrinsic cells is less clear. This issue is relevant in the light of the recent results obtained in animal models, showing that cells recruited from circulation (i.e. inflammatory cells) reside in the graft intima, where they may activate vessel-resident cells or directly differentiate into SMCs, or that vesselresident progenitors are triggered to differentiate 140 CCM — Scientific Report 2011 — Ongoing research 2012 into SMCs by signaling associated to vascular injury/ mechanical stress. Vascular progenitors endowed with clonogenic potential and differentiation ability have been recently found into human SVs. These cells, named saphenous vein progenitors (SVPs), can be grown ex vivo from expansion of primary CD34+CD31- cells obtained from enzymatic digestion of SV segments. To assess the role of biomechanics in possible SVP-mediated phenotype changes, we have performed stimulations with a commercially available bioreactor (FlexCell System), using a custom made bioreactor platform tailored to perform vessel conditioning in an organ culture condition. Use of these tools showed a crucial role of biomechanics in SVPs differentiation and growth control, as well as in changes of vein structure and remodeling. This research is performed by our Laboratory in collaboration with the Dept of Biomedical Engineering of the Politecnico of Milan, and the Laboratory of Regenerative Medicine of the Bristol Heart Institute, Bristol, UK. Analysis of the interaction between stem cells and biopolymers using high-throughput screening techniques: towards engineering of the artificial cardiovascular stem cell niche. (Fig. 3) Recent integration of the high content imaging platforms with the “micro-patterning” (e.g microcontact- or inkjetprinting) techniques has allowed emergence of a new bioengineering branch tailored to study (stem) cell behavior under condition of confinement into geometrically defined or chemically definite composed micro-environments. In addition, reproduction of physiological or pathological mechanical forces in micrometer scale by use of the so called “lab-on-chip” fabrication philosophy, allows stem cells interrogation for multiple basic responses (differentiation, proliferation, markers modulation, modifications in the epigenetic landscape) to complex and combinatorial environmental conditions, in a single experimental setting. In the present project, the interactions between cardiac- derived c-kit+ cells and of the so called valve interstitial cells (VICs) onto polymer arrays is currently being analyzed making use of this recent approach. This will lead to identify the best polymers to grow cardiac and valve derived progenitors with “niche”-compliant conditions. The final result will be the formulation of “smart” materials to instruct auto-assembly of myocardial tissue and aortic valve artificial leaflets with native-like properties. This research, is carried by our laboratory in collaboration with the Laboratory of High Throughput Chemistry of the University of Edinburgh, UK. Decellularization of the human pericardium: towards the generation of a biocompatible scaffold for aortic valve tissue engineering. (Fig. 4) Engineering of aortic valve (AoV) leaflets with characteristics of native tissue is an important step toward derivation of AoV implants with maximal CCM — Scientific Report 2011 — Ongoing research 2012 141 Fig. 3 Fig. 4 INKJET-PRINTING/CHIP ARCHITECTURE AND DESIGN 13x16 polymers grid Fresh Spot shape, pitch and dimensions MICROCONTACT PRINTING (μCP)/CELL CULTURE biological compliance and durability. This might be advantageous compared with the use of animal-derived bio-prosthetic valves, donor-derived homografts, or mechanical valves. This possibility is particularly attractive for pediatric AoV surgery. In fact, pediatric patients need to be transplanted with valve tissues able to grow in concert with the heart, thereby generating durable grafts that do not need further substitution during the life span. Pericardium from different animal species has been introduced to generate the so called bio-prosthetic valves. The major limitation of these devices is that aldehyde fixation, commonly used to prepare pericardium of animal origin, causes calcification and mechanical failure over time due to the absence of an active cellular machinery necessary for remodeling and renewing extracellular matrix components and the presence of cellular remnants, which act as a calcium “nucleation” centers. We have setup a method to 142 CCM — Scientific Report 2011 — Ongoing research 2012 Decellularized decellularize the human pericardium using hypotonic buffers preserving mechanical resistance of the tissue in strain-stress tests, also after cryo-preservation. Further, decellularized pericardium was implanted subcutaneously for up to two months into immunocompetent mice, to analyze rejection and calcification. The results showed that decellularization using the adopted method, with or without cryopreservation, granted an optimal tolerance of the human tissue. This research is performed by our laboratory in collaboration with the Dept of Biomedical Engineering of the Politecnico of Milan, the Dept of Pharmacology of the University of Milan and the Cardiovascular Tissue Bank at Centro Cardiologico Monzino. 40x 40x 40x 40x 20x 20x Publications Burba I, Colombo GI, Staszewsky LI, De Simone M, Devanna , Nanni S, Avitabile D, Molla F, Cosentino S, Russo I, De Angelis N, Soldo AR, Biondi A, Gambini E, Gaetano C, Farsetti A, Pompilio G, Latini R, Capogrossi, MC, Pesce M. Histone Deacetylase inhibition enhances self renewal and cardioprotection by human cord bloodderived CD34+ cells. PLoS One 2011;6(7): e22158 Cheema FH, Polvani GL, Argenziano M, Pesce M. Combining stem cells and tissue engineering in cardiovascular repair – a step forward to derivation of novel implants with enhanced function and self renewal characteristics. Recent Pat. Cardiovasc. Drug Discov. 2012;7(1): 10-20 perspectives from pericardium? IBiomaterials and Stem Cells in regenerative Medicine (Murugan Ramalingam, Seeram Ramakrishna and Serena West Eds),2012, CRC-Press Pesce M, Pompilio G, Polvani GL, Capogrossi MC. When Stemness meets Engineering: towards “Niche” Control of Stem Cell Functions for Enhanced Cardiovascular Regeneration. In (Gustav Steinhoff Ed.), Regenerative medicine (Second Edition). Springer 2012 Vinci MC, Polvani GL, Pesce M. Epigenetic programming and risk: the birthplace of cardiovascular disease? Stem Cell Rev Rep, 2012 Vinci MC, Prandi F, Micheli B, Tessitore G, Guarino A, Dainese L, Polvani GL, Pesce M. Natural membranes as scaffolds for biocompatible aortic valve leaflets: CCM — Scientific Report 2011 — Ongoing research 2012 143 Plasma and Gene Bank The bank collects plasma and genes from patients undergoing aortocoronary bypass grafts (CEC or no CEC) in order to develop research on cardiovascular risk factors Clinical Research DNA Bank Since 2002, a genomic DNA bank collecting DNA from patients affected by coronary diseases and/ or other atherosclerotic pathologies as well as from healthy patients, has been established at Centro Cardiologico Monzino in order to investigate markers (polymorphisms) useful both in the identification of cardiovascular risk factors and in the characterization of acute vascular events in high risk subpopulations. The DNA bank is connected to a database which collects the patient clinical information allowing the identification of subjects with specific characteristics (age, gender, family history, etc…). In the last years the bank has turned out to be a precious help in carrying out studies concerning the development and progression of atherosclerotic pathology in patients with candidate gene polymorphisms 144 CCM — Scientific Report 2011 — Ongoing research 2012 CCM — Scientific Report 2011 — Ongoing research 2012 145 Relationships between heart and kidney function in acute cardiovascular conditions 146 CCM — Scientific Report 2011 — Ongoing research 2012 disease and acute kidney injury have been carried out at Centro Cardiologico Monzino, in collaboration with the Interventional Cardiology and the Post-Operative Intensive Care Units. The goal of these studies is to characterize, in terms of acute kidney injury risk and associated morbidity and mortality, subsets of patients undergoing interventional coronary procedures or cardiac surgery. The clinical scenarios considered in this area of research were ST-elevation acute myocardial infarction (STEMI) and cardiogenic shock treated with primary percutaneous coronary intervention, severe renal insufficiency (stage IV and V of the classification proposed by the National Kidney Foundation) undergoing elective cardiovascular procedures, and chronic kidney disease patients undergoing cardiac surgery. All these patients have been identified as at very high risk for acute kidney injury and poor outcomes, because of the presence of multiple comorbidities and of additional factors, other than contrast exposure (hemodynamic instability, bleeding, cardiopulmonary support, nephrotoxic drugs, etc.), that may negatively impact on kidney function. The combination of these factors increases the development of cardiac disease, contributes to progression of renal dysfunction, and ultimately perpetuates mortality risk. New prophylactic strategies for renal protection have been prospectively evaluated in these highrisk populations. They are based on pharmacological (N-acetylcysteine), mechanical (hemofiltration), or combined (furosemide-induced diuresis with matched hydration) approaches. The general concept emerging from these studies is that no universal strategy for renal protection exists. Indeed, several lines of preventive therapy are possibly required, and the best therapeutical option should be selected on the bases of the single patient’s risk profile and the considered clinical setting. As the poor prognosis associated with renal insufficiency may partially, or totally, thwart the benefit obtained by percutaneous or surgical coronary No AKI AKI Stage 1 AKI Stage 2-3 57% 60 50 In-hospital mortality (%) A large body of experimental and clinical evidences, as well as an increasing awareness, indicates that both chronic kidney disease and acute kidney injury are relevant issues in cardiovascular medicine from an epidemiological, clinical, and prognostic point of view. Diagnosis and treatment of patients with cardiovascular disease rely heavily on cardiovascular imaging and on interventional coronary procedures and cardiac surgery. Contrast-mediated imaging studies and interventions are a relevant part of modern medical practice. An increasing number of patients, estimated at 30 million per year in the United States, receive contrast agents during diagnostic or interventional procedures. Iodinated contrast media have a strategic place in this expanding field and, although they are essential for contrast enhancement and diagnostic precision, they are also toxic for the kidney. Indeed, one of the most troublesome complications of contrast agent administration is kidney toxicity, and contrast-induced nephropathy represents one of the leading causes of renal impairment and the third cause of in-hospital acquired renal failure. Development of contrast-induced nephropathy is linked to a higher risk of cardiovascular complications, prolonged hospitalization, and increased in-hospital and long-term mortality. Acute kidney injury is also a common complication after cardiac surgery, associated with significant morbidity and mortality, and with a prolonged intensive care unit and hospital stay. Temporal trends in cardiac surgery show that patients with co-morbidities and complex surgical procedures are increasing. Thus, acute kidney injury after cardiac surgery is an important health problem that is expected to increase in incidence. Therefore, the effective prevention of renal deterioration, particularly in patients with preexisting renal insufficiency, should improve morbidity and mortality following percutaneous coronary procedures and cardiac surgery, and decrease hospital stay and costs. In recent years, several studies on chronic kidney 43% 40 30 22% 20 0 12% 9.5% 10 6% 1% N=2801 1.3% N=262 N=147 Overall population 0% N=1467 N=155 STEMI N=181 N=1339 N=104 N=64 NSTEMI/UA In-hospital mortality in patients with acute coronary sindromes, developing, or not (no AKI), mild (Stage 1) and severe ( Stage 2-3) acute kidney injury (AKI). STEMI = ST-elevation acute myocardial infarction; NSTEMI = non-ST-elevation acute myocardial infarction. revascularization, exploration of promising new strategies continues, with the hope that pharmacological or mechanical kidney protection might improve outcomes in these patients. Finally, alternative non pharmacological approaches for the therapy of acute and chronic heart failure have been investigated. In collaboration with the Heart Failure Unit, large experience has been acquired in the treatment of patients with refractory congestive heart failure and severe fluid overload by means of different kind of renal replacement therapies, in particular ultrafiltration and hemofiltration. CCM — Scientific Report 2011 — Ongoing research 2012 147 Candidate biomarkers for the clinical and prognostic stratification of patients with acute coronary syndromes 148 CCM — Scientific Report 2011 — Ongoing research 2012 Inflammatory prothrombotic biomarkers. Several research activities are ongoing, regarding the Course after hospital presentation for CK-MB and serum cytochrome c in STEMI patients treated with primary angioplasty. Data are presented as median and interquartile range. 250 CK-MB (ng/mL) Citochrome c. In collaboration with the Experimental Oncology Department of Istituto Europeo di Oncologia (IFOM-IEO), the Intensive Cardiac Care Unit is evaluating serum levels of cytochrome c, a mitochondrial protein, as a potential marker of apoptosis associated with myocardial reperfusion injury in STEMI patients. Primary percutaneous coronary intervention is the most effective strategy for reducing infarct size and improving clinical outcomes in patients presenting with a STEMI. The process of myocardial reperfusion, however, can induce injury to the myocardium caused by the abrupt restoration of coronary blood flow after an ischemic episode, thereby reducing the beneficial effects of myocardial reperfusion. Indeed, reperfusion-induced myocardial injury has been experimentally shown to induce cardiac cells death and to increase infarct size, accounting for up to 50% of its final size. Several studies have generated interest in the reperfusion phase of STEMI, as a possible target of cardioprotection. Until recently, however, the efficacy shown by most cardioprotective agents in animal models, has been difficult to confirm in clinical trials. One possible reason is the lack of available biomarkers of reperfusion injury that allow us to detect in clinical practice the presence of reperfusion-induced myocardial damage, to measure its extent, and to evaluate the effects of cardioprotective interventions. Myocardial reperfusion injury is mainly due to apoptotic cell death that occurs in response to oxidative stress, ATP depletion and other stimuli triggered by restoration of blood flow after coronary occlusion. Mitochondrial cytochrome c release is a key event in the activation of caspase-3, a downstream pivotal step of early stages of apoptosis. Thus, cytochrome c concentration in plasma of patients with STEMI represents a possible new index of apoptotic cell death associated with coronary reperfusion, and its measurement could provide important clinical, prognostic, and therapeutic information in this setting. Recently published data (Marenzi G. et al. Am J Cardiol 2010) seem to confirm this hypothesis; further investigations on a larger population of patients with acute coronary syndromes are ongoing to establish the possible complementary prognostic value of this marker, when considered together with classical indexes of myocardial necrosis. 200 characterization of genomic, proteomic, thrombotic, and inflammatory profiles of patients with acute coronary syndromes (for details see the research activities of the Laboratory of Biology and Biochemistry of Atherothrombosis). In these patients the mechanisms underlying the association between high risk clinical features and enhanced mortality have not been fully elucidated but are possibly associated with the presence of an abnormal pathological background, including platelets activation and coagulation processes, inflammatory response, and cellular characteristics and functions. We investigate the biological aspects that distinguish low from high risk patients with acute coronary syndromes, in terms of thrombotic, inflammatory, and cellular characteristics, oxidative stress and nitric oxide pathway. The acquisition of a new knowledge about the complex substrate underlying high risk patients suggests new therapeutic targets and strategies aimed at significantly reducing the increased mortality rate of these patients. Vitamin D deficiency. Recent studies have highlighted the role of vitamin D deficiency in a variety of basic biological and physiological processes throughout the body, including the cardiovascular system. Accumulating 150 100 evidences suggest that vitamin D levels in plasma are lower in the presence of cardiovascular risk factors such as diabetes, hypercholesterolemia, hypertension, and chronic kidney disease, and that vitamin D deficiency is associated with an increased cardiovascular risk. Vitamin D deficiency might also play a role in the pathogenesis of acute coronary syndromes (ACS). However, no information is available on the levels of vitamin D in blood of patients hospitalized with ACS, as well as their relationship with disease severity and short-term clinical outcome. Recognition of the mechanisms linking vitamin D deficiency to increased mortality risk in ACS patients is a critical challenge which might justify a strategy based on “acute vitamin D supplementation” as a novel effective therapy for high-risk ACS patients. A new research project is ongoing, promoted by the Intensive Cardiac Care Unit, in collaboration with the Nephrology and Dialysis Unit, Multimedica IRCCS, the Laboratory of Biology and Biochemistry of Atherothrombosis and the Clinical Chemistry Unit. The project is aimed at investigating the role of vitamin D deficiency in the setting of ACS, its relationship with in-hospital outcomes, and its possible influences on platelet function and thrombus formation. 50 0 0 6 12 18 24 30 36 48 72 96 0 6 12 18 24 30 36 48 72 96 hours 2,0 Cytochrome c (ng/mL) Research activity is focusing on the study of new possible biomarkers to be used for clinical characterization and prognostic stratification of patients with acute coronary syndromes. 1,5 1,0 0,5 0,0 hours CCM — Scientific Report 2011 — Ongoing research 2012 149 Cardiopulmonary pathophysiology Lung functional abnormalities. It is now well known that lung function abnormalities are part of the chronic heart failure syndrome, as both lung mechanics and gas exchange are impaired. Impairment of lung mechanics is Pulmonary function in patients grouped in 4 functional classes according to peak VO2 120 100 80 VO2 Max <12 ml/Kg/min VO2 Max 12-16 ml/Kg/min VO2 Max 16-20 ml/Kg/min VO2 Max >20 ml/Kg/min ° == pp << 0.01 * 0.01 ° ° ° ° ° ° * ° ° 60 40 20 0 150 FVC (%) FEV1 (%) FEV1/FVC CCM — Scientific Report 2011 — Ongoing research 2012 MVV present at rest in patients with severe HF. However, lung mechanics abnormalities are evident, even in patients with moderate HF, during physical activity. Indeed, at rest, pulmonary function is normal in patients with moderate HF whereas a restrictive lung disease is frequently observed in patients with severe HF. We have grouped in four classes HF patients according to exercise capacity and identified a restrictive lung disease in patients with peak VO2 < 12 ml/min/kg and a strong tendency toward a restrictive lung disease in HF subjects with an exercise capacity ranging between 12 and 16 ml/min/kg Cardiac enlargement and lung fluid increase are among the major causes of the restrictive lung disease. Indeed, we showed an inverse relationship between cardiac volume and pulmonary function. Lung function abnormalities during exercise. In an international multicenter collaborative study it has been shown that, at a given VO2, the higher the ventilation the greater the HF severity. The increase of ventilation is due to an increase in respiratory rate with the tidal volume being lower in patients with severe heart failure. In figure 1a, VO2 is plotted vs VE. Data show that for the same VO2, patients in a lower functional class have a higher ventilation than normal subjects or patients with less severe heart failure. In figure 1b, VE is increased due to an increase of respiratory rate with a lower tidal volume in more compromised patients. We have also shown that heart failure patients, at variance with normal subjects, have a reduced residual functional capacity (FRC) at the beginning of exercise but, when they reach an early expiratory flow limitation, they increase FRC in order to increase ventilation. The increase in FRC and both the reduced expiratory time and the presence of uneven lung compliance, produce disomogenity of end-expiratory alveolar pressure which leads to ventilation/perfusion inhomogeneity. Finally, we published a paper about the evolution of the Fig. 1a concept of ventilatory limitation during exercise combining the pneumologist and cardiologist point of view. Lung diffusion abnormalities in chronic HF patients. In humans, alveolar gas exchange is measured in terms of total lung diffusion for carbon monoxide (DLCO) and specific membrane diffusion capacity (Dm). We have suggested that DLCO abnormalities have a prognostic capacity in HF, are a target for therapy and also a limiting factor for exercise performance. Indeed, heart failure patients with low DLCO have a reduced exercise capacity. For a given VO2 the oxygen pressure gradient across the alveolar capillary membrane has to increase more than in subjects with normal DLCO. Consequently, when exercise is performed below sea level, as in the Dead Sea, or at a high altitude, HF subjects with reduced DLCO improve or reduce their exercise performance more than HF patients with normal DLCO. DLCO and DM abnormalities have a relevant prognostic capacity in HF albeit it is yet unknown whether or not the improvement of DLCO obtained with treatment is associated with an improvement of prognosis. Fig. 1b We have done several high altitude experiments using a simulated altitude model which has been developed at Centro Cardiologico Monzino/Department of Cardiovascular Science, Milano University, as well as participating to a Highcare International Research Mount Everest Expedition (http://www.highcare2008.eu/). There is a linear correlation between DLCO and peak VO2 Peak VO2 Over the last twenty years the Cardiopulmonary Research Laboratory at Centro Cardiologico Monzino has played a major role in research advancement in the understanding of cardiopulmonary interaction in heart failure (HF). This has been made possible by the strong collaborative network with the Emergency Unit for BNP (natriuretic peptide) and pulmonary edema studies, with the Intensive Cardiac Care Unit for ultrafiltration studies, with the Interventional Cardiology Unit for coronary angiography, with the Electrophysiology Unit for biventricular pace makers, with the Anaesthesiology and Intensive Care Unit for cardiopulmonary interaction in the operating room, with the Echocardiography and Radiology Units for echo and TC studies and with the Laboratory of Biology and Biochemistry of Atherothrombosis for the identification of biomarkers of disease, e.g. metalloproteasis, surfactant derived proteins etc. CCM — Scientific Report 2011 — Ongoing research 2012 151 Moreover, we performed several studies on gas exchange abnormalities in HF and have identified the first biomarker of alveolar capillary membrane damage. Indeed, we reported an increased circulating plasma level of surfactant protein B (SPB) in HF patients whose value is higher when HF is severe. SPB level correlates with lung diffusion, both total DLCO and membrane specific Dm, and with peak VO2 and VE/ VCO2 slope. Gas exchange abnormalities are associated with anatomical changes in the alveolar-capillary membrane, which include reduction in the number of the alveolarcapillary units, interstitial fibrosis, local thrombosis and an increase in cellularity. All this has been extensively studied in our laboratory elaborating two heart failure models (rapid saline infusion and hypoxia exposure, both with reducing FiVO2 and with high altitude exposure) and demonstrating the active role on DLCO in HF of several therapeutic interventions: increase in DLCO by ACE-inhibitors, anti-aldosteronic drugs, a during exercise, is associated to a reduction in DLCO which is greater when the HF severity is serious. We have now a more clear understanding of gas diffusion in heart failure patients thanks mainly to our twenty five years studies at the Cardiopulmonary Research Laboratory of Centro Cardiologico Monzino. Several research studies are still ongoing or under development. Artero-venous difference vs cardiac output for different peak VO2, measured with rebreathing and with Fick 20 18 16 VO2 3 14 2,5 12 2 10 neutral effect by ultrafiltration and AT1 blockers, and a negative role by B1.B2 receptors blockers (carvedilol). We have also shown that the capillary blood volume at rest is reduced in patients with severe exercise limitation and that reduction of lung fluids by ultrafiltration is not associated to DLCO improvement. Differently a transitory increase in pulmonary vascular pressure, as it happens CO determination during exercise. We are now capable to measure simultaneously during exercise cardiac output, VO2 and the artero-venous O2 differences, in other words to split the Fick equation into its three components. Clinically this allows to understand and separate from each other, in HF patients, the role of anaemia, muscle deconditioning, and cardiac output reduction guiding us in a data based decision on CRT, drug and surgical treatment. New insights are now available on exerciseinduced blood-flow redistribution before and after training. 1,5 8 1 Rebreathing 6 0,5 Flick 4 2 0 0 2 4 6 8 10 12 14 16 18 C(a-v)O2 estimated/measured (ml/100ml) DLCO and its components, Dm (membrane diffusion capacity), Vc (capillary volume) and Va (alveolar volume), in different functional class. 152 CCM — Scientific Report 2011 — Ongoing research 2012 CCM — Scientific Report 2011 — Ongoing research 2012 153 Interventional Cardiology The Interventional Cardiology Unit is involved in several lines of clinical research focusing on the percutaneous treatment of coronary artery disease, peripheral vascular disease and structural heart disease. The aim of our scientific work is to improve treatment outcome by means of new transcatheter techniques and innovative interventional devices and to explore innovative diagnostic modalities in the area of coronary and peripheral atherosclerotic disease. Coronary artery disease The Unit is in the vanguard in the area new coronary stent evaluation, investigating the efficacy of second generation drug-eluting stents (DES) and assessing the clinical outcome of DES use for off-label indications in percutaneous coronary intervention (PCI). New coronary stents. Currently available stents were designed for straight lesions in which they have shown to provide superb acute and long-term results. One lesion subset that continues to challenge the interventional cardiologist is bifurcation lesions. A number of different strategies have been employed with standard stents to address bifurcation lesions each of which has significant limitations including decreased procedural success and increased restenosis and thrombosis rates. These limitations prompted the development of stents designed specifically to treat bifurcation lesions. We are currently evaluating the Tryton Side-Branch Stent™, a cobalt chromium balloon expandable stent designed specifically for bifurcation lesion treatment. The aim is to assess the safety and feasibility of the Tryton Side-Branch Stent™ in this lesion subset and to evaluate in detail intravascular ultrasound findings immediately after stent deployment and at six-month follow-up in order to correlate them with clinical outcome. Second-generation DES. Few data substantiate long-term safety and efficacy of second-generation DES in the real- 154 CCM — Scientific Report 2011 — Ongoing research 2012 world. We are enrolling real-world patients and coronary lesions in our registry to assess acute, mid-term (6 months) and long-term (2 year) outcome of two second generation DES, the EndeavorTM-zotarolimus-eluting stent and the Xience VTM-everolimus eluting stent. Moreover, we are involved in a multicenter randomized trial (Spirit women randomized trial) comparing a first generation DES, the Cypher sirolimus eluting stent, with a second generation DES, the Xience VTM-everolimus-eluting stent, in women. Bioabsorbable Vascular Scaffold (BVS). We started for the first time in Italy a clinical study for the assessment of the safety and performance of the BVS, a novel polymeric bioabsorbable stent in patients with obstructive coronary artery disease characterized by a maximum of two de novo native coronary artery lesions each located in different epicardial vessels. The BVS is comprised of 4 main components: an anti-proliferative drug (everolimus), expected to be 80% eluted by 28 days, a polymer drug reservoir, expected to be fully absorbed in 9 months and a polymer stent, expected to be fully absorbed in 18 to 20 months. The BVS, despite being a polymer that is naturally absorbed and fully metabolized, performs like a metallic DES in terms of deliverability, conformability and scaffolding. The key advantages are that it leaves behind, after bioabsorption, a healed natural vessel without any permanent implant and is fully compatible with MDCT imaging. Off-label use of DES. We are participating in the GISESICI registry, an ongoing retrospective observational multicenter registry promoted by the Italian Society of Invasive Cardiology, in which 19 high-volume centers enrolled 1,453 consecutive patients who underwent percutaneous coronary intervention on unprotected left main coronary artery. The aim is to compare long-term clinical outcome following DES or bare-metal stents (BMS) implantation on lesions located at the ostium, the shaft or the bifurcation of the left main in a large realworld population. In this registry, the risk of ischemic events in relation to the duration and time of suspension of dual antiplatelet therapy is also assessed as well as the impact of acute coronary syndrome, gender, left ventricular function and diabetes on mid- and long-term outcome. Another field of interest is the implantation of longer and multiple overlapping DES in diffusely diseased vessels, as well as total vessel reconstruction. These interventions are increasing in daily clinical practice in relation to the significant decrease of restenosis rate after DES implantation even in very complex coronary lesions. Recently, however, concerns have been raised regarding the safety of DES use in off-label indications such as very long lesions, especially with regards to the risk of late and very late stent thrombosis, often coinciding with the cessation of one or both antiplatelet agents. Therefore, we are conducting a study that is aimed at the evaluation of all patients who underwent long lesions stenting with a first-generation sirolimuseluting DES (Cypher) since its introduction in our institution (April 2002). Data were collected from a prospectively created database in which the specific target stents length, longer stented length (>60 mm) subgroup and clinical follow-up were decided prior to data interpretation. Analysis of these data will provide critical information regarding the safety and effectiveness of multiple and overlapping implantations of this specific DES in patients with long and diffuse coronary artery disease. Acute myocardial infarction. Several randomized trial have demonstrated that primary angioplasty is the more effective reperfusion modality in acute myocardial infarction resulting in fewer deaths, reinfarctions and strokes than fibrinolysis does. One limitation of primary PCI is the “no-reflow phenomenon”, a dire event defined as the inability to perfuse a portion of myocardium after re-establishment of patency of a previously occluded epicardial coronary artery. No-reflow is associated with myocardial injury, lack of myocardial function recovery and increased mortality. We are focusing our research activity on the prevention and management of the no-reflow phenomenon in acute myocardial infarction patients undergoing primary PCI. Use of innovative distal protection and thrombus aspiration devices, in order to prevent distal embolization, and specific pharmacological treatment approaches for preservation of the coronary microcirculation function are currently evaluated in this clinical setting. Stress cardiomyopathy (Tako-Tsubo syndrome). This is a relatively rare but dramatic acute cardiac condition that mimics myocardial infarction and is mostly observed in women. We are exploring the pathogenesis and triggers of the Tako-Tsubo syndrome, as well as the therapeutic strategies and long-term outcome. Unstable coronary plaque. Propensity of subcritical coronary artery plaques to induce acute coronary events is investigated by intravascular virtual histology technique (VH-IVUS). This technique allows the differentiation between stable fibrotic plaques, which do not require invasive treatment, from plaques filled with lipid components that may be prone to abrupt rupture and able to trigger an acute coronary syndrome. Detection and categorization of subcritical unstable coronary plaques using VH-IVUS in order to correlate them with clinical outcome and their passivation by stenting represent specific field of research. Peripheral interventions Carotid stenting. This field of research is based on an interventional experience in almost 600 patients who were treated with carotid stent implantation using different types of stents and brain protection devices. The clinical results compare very favorably with those CCM — Scientific Report 2011 — Ongoing research 2012 155 reported in the literature and the standard of care requirements of the scientific societies for the treatment of carotid artery disease. Areas of clinical research in this field include: a)The comparison of different types of brain protection devices (distal vs. proximal protection) and carotid stenting (CAS) technique (predilation vs. direct stenting), and evaluation of the clinical value of trans-cranial Doppler monitoring during CAS in high-risk patients. b)The investigation of CT-angiography role as a pre-CAS diagnostic assessment tool to identify patients at high anatomical risk for cerebral complication or CAS failure c)The comparison between CT-angiography and Doppler US in the assessment of stenosis severity and composition d)The study in detail of intracranial circulation variant in relation to patient tolerance of a proximal protection device (MoMa). Comparative evaluation of invasive vs. non-invasive coronary artery imaging techniques. With the introduction of multidetector computed tomography (MDCT), coronary computed tomography (CT) angiography has emerged as a new tool for diagnosing coronary artery disease and patient followup. We are involved in several studies in collaboration with the Area of Cardiovascular Imaging aimed at assessing the diagnostic performance, as compared to invasive coronary angiography, of 64-slice MDCT for the detection of coronary stenosis in patients with low probability of coronary artery disease such as patients with dilated cardiomyopathy. Other studies focus on the feasibility and diagnostic accuracy of 64-slice MDCT for the evaluation of in-stent restenosis comparing the finding of this non-invasive imaging modality to the results of invasive coronary angiography and intravascular ultrasound in patients who were 156 CCM — Scientific Report 2011 — Ongoing research 2012 previously treated with coronary stent implantation. Moreover, we are assessing the prevalence of coronary artery anomalies in patients who undergo MDCT and correlating the MDCT anatomical findings to the patient clinical symptoms. The aim is to assess in which cases MDCT has an additional clinical value compared to invasive coronary angiography in the diagnosis and characterization of these congenital pathologies. Structural heart disease Atrial septal defect and patent formane ovale. Since 2000, our Unit has been involved in the percutaneous treatment of atrial septal defect (ASD) and patent foramen ovale (PFO) patients. A causal relationship between PFO and migraine has been recently hypothesized. Indeed, increased frequency of PFO in migraineurs was first reported in 1998 in a case-control study and PFO has a prevalence of 15% to 25% in the general population and up to 60% in patients with migraine with aura. In consideration of the reports of several retrospective uncontrolled studies that have indicated improvement of migraine with aura after percutaneous PFO closure, we are prospectively assessing, using a validated migraine severity score, the impact of PFO closure on migraine attacks over time in consecutive patients who were treated with the Amplatzer PFO occluder in our institute since May 2000. Mitral valve regurgitation. Mitral regurgitation affects millions of patients worldwide, yet only about 20% of the 600,000 patients diagnosed in the United States and Europe each year undergo open heart surgery, the traditional treatment for mitral regurgitation. We are conducting a clinical study with a new device (MitraClip system) for non-surgical repair of mitral valve regurgitation. This breakthrough mitral valve repair technology clips the leaflets of the mitral valve together to reduce regurgitation offering a minimally invasive alternative to open heart surgery – not unlike the opportunity that stents provided more than two decades ago for the treatment of coronary artery disease. In 2011, we are continuing a clinical study to assess the safety, feasibility and efficacy of this new interventional treatment approach in patients with severe mitral regurgitation considered high risk for mitral valve surgery. therapy at 1 and 6 months after thienopyridine suspension. As a comparison, we are analyzing platelet activation in 20 medically-treated stable angina patients. Therapeutic renal denervation We initiated a study to evaluate the safety and blood pressure-lowering efficacy of selective renal denervation using a novel percutaneous, catheter-based treatment in patients with difficult to-control and resistant hypertension. In this approach, renal sympathetic nerve ablation is achieved percutaneously via the lumen of the main renal artery using a catheter connected to a radiofrequency (RF) generator. After gaining access via the femoral artery and confirmation of anatomic eligibility with renal angiography, the treatment catheter (Symplicity, Ardian, Inc) is introduced into each renal artery, and discrete RF ablations lasting ≤2 minutes each are applied to achieve ≤6 ablations separated both longitudinally and rotationally within each renal artery. Catheter tip temperature and impedance are constantly monitored during ablation, and RF energy delivery is regulated according to a predetermined algorithm. Antiplatelet therapy and platelet function inhibition after drug-eluting stent implantation Discontinuation of antiplatelet therapy, in particular thienopyridine withdrawal, has emerged as one of the most important predictors of stent thrombosis. In this regard, a rebound effect has been suggested to be responsible for the adverse events reported within the initial 90 days after stopping clopidogrel in patients previously treated with DES implantation. In collaboration with the Unit of Cell Biology and Biochemistry of Atherothrombosis, we are evaluating patients treated with DES who underwent evaluation of platelet activation markers during dual antiplatelet CCM — Scientific Report 2011 — Ongoing research 2012 157 Electrophysiology Area: scientific hot topics Our recent research efforts are mainly focused on: a) catheter ablation of atrial fibrillation; b) catheter ablation of life-threatening ventricular arrhythmias; c) substrate mapping and diagnostic endomyocardial biopsy in different subsets of cardiomyopathy; d) new techniques to achieve clinically significant reduction of the exposure to ionizing radiation in supraventricular tachycardia ablation; e) identification of the best strategies for left ventricular stimulation in patients implanted with biventricular pacemaker and/or cardioverter defibrillator. f) evaluation of the multielectrode pulmonary vein isolation system for the treatment of paroxysmal atrial fibrillation (REVOLUTION Study) g) Advantages of a novel surround-flow irrigated catheter for ventricular tachycardia ablation (THERMOCOOL SF Study) Atrial fibrillation (AF) is the most common significant cardiac arrhythmia, responsible for approximately onethird of all hospital admissions of patients suffering from cardiac rhythm disturbances. It is responsible for an increased risk of stroke, heart failure and all-cause mortality. Over the last decade the vast improvement in the long term efficacy of catheter ablation, compared to pharmacological treatment, supports the use of ablation in the early management of patients suffering from atrial fibrillation. The success rate of AF ablation varies between 65% and 85% in patients with AF, depending on type of AF (paroxysmal or persistent or permanent), patient selection, technique used, and methods of follow up. Our research activities are aimed at identifying 1) the biochemical and structural predictors of AF, and 2) the procedural techniques associated with improved success rates of catheter ablation procedures, particularly in patients with persistent AF. Regarding biochemical predictors of AF, the recent rapid evolution of microRNA (miRNA) research has shown that 158 CCM — Scientific Report 2011 — Ongoing research 2012 this class of small non-coding RNAs plays important roles in diverse fundamental biological processes including cell growth, differentiation, aging and death. In particular some of these miRNAs have been shown to be involved in AF and are considered to have the potential to regulate AF based on their target genes. Thus aim of our studies is the identification of tissue or circulating miRNAs in young patients suffering from AF in the absence of any apparent predisposing cause. Another research thread is the study of atrial fibrosis identified by cardiac MRI and low potentials on electroanatomical atrial substrate mapping. To this regard an analysis will be performed to determine whether the presence or absence of atrial fibrosis influences the long-term efficacy of catheter ablation. In the first of our ongoing studies on procedural techniques, we are testing a “step-wise” AF ablation strategy to improve the effectiveness of the procedure in patients with persistent AF. Patients undergo catheter ablation guided by 3D electroanatomical mapping systems (CARTO 3), with the aim of electrically isolating pulmonary veins, and performing left atrial substrate modification by means of ablation of complex fragmented atrial electrograms and linear ablation on the left atrial roof, left mitral isthmus, right cavotricuspid isthmus. The follow-up of these patients is strictly based on data recorded from a loop recorder implanted immediately after ablation. These patients also undergo a functional cardiac evaluation, by means of cardiopulmonary exercise testing and non-invasive measurement of cardiac output at baseline and during exercise. The aim is to evaluate whether persistent AF compromises cardiac function even in cases with no overt reduction in left ventricular ejection fraction. Another topic of our research activity is the evaluation of new mapping and ablation catheters to electrically isolate the pulmonary veins in patients with paroxysmal AF. The catheters under study in our laboratory use different sources of ablation energy, including radiofrequency, extreme cold (cryoablation) and laser energy. We are also studying genetic determinants predisposing to intra-atrial thrombus formation in patients with persistent AF despite regular oral anticoagulant therapy (i.e. INR between 2 and 3). Previous studies conducted in our echocardiography laboratory demonstrated that 6-7% of patients undergoing a transoesophageal echocardiogram before electrical cardioversion have intra-atrial thrombus despite a correct value of INR. Blood samples are also obtained from patients who undergo transoesophageal echocardiography before electrical cardioversion to evaluate possible genetic determinants predisposing to thrombus formation. Ventricular arrhythmias. Radiofrequency catheter ablation is now considered a curative approach for ventricular tachycardia (VT), either idiopathic or in the setting of ischaemic or non-ischaemic cardiomyopathy. In our Electrophysiology laboratory, the success rate of VT ablation approximates 70%. However, management of recurrent VT often remains difficult, as in some patients neither antiarrhythmic drugs nor conventional endocardial radiofrequency ablation can prevent all recurrences. Ongoing research of the Electrophysiology Area is focused on the possibility to improve the success rate of VT ablation by means of different 3D mapping systems, often integrated by intracardiac echocardiography of the ventricular chambers. Figure 1. Primary and secondary cure rates (freedom from atrial fibrillation recurrence) in 1404 patients undergoing pulmonary vein antrum isolation guided by a circular mapping catheter and intracardiac echocardiography at 4 different Institutions with 12 different operators. P<0.001 % 100 90 80 70 60 50 40 30 20 10 0 P=0.006 92,2 77,6 P=0.28 86,4 83,3 75,8 60,6 Paroxysmal Persistent Primary cure rate Permanent Secondary cure rate CCM — Scientific Report 2011 — Ongoing research 2012 159 One of our studies on VT ablation aims to evaluate the impact on success rate of catheter ablation of a software for automated pace-mapping (PaSo) in patients with frequent ventricular premature beats. Coupled with standard electroanatomic CARTO mapping, the PaSo software can perform automated template matching, which helps to localize the optimal ablation site of ventricular premature beats arising from either the left or right ventricle. Another ongoing trial is aimed at evaluating the usefulness of intracardiac echocardiography of the left ventricle integrated with 3D electroanatomic mapping (CartoSound). Intracardiac echocardiography is possible because lower-frequency transducers have been miniaturized and mounted onto catheters which can be inserted transvenously into the heart. These lower-frequency transducers are capable of enhanced tissue penetration, permitting high-resolution 2D “whole-heart” imaging. Intracardiac ultrasound may facilitate electrophysiological procedures and VT ablation by guiding trans-septal catheterization, enabling visualization of endocardial anatomy and more precise targeting of arrhythmogenic substrates, ensuring optimal ablation electrode/tissue contact and promptly diagnosing procedural complications. A third ongoing multicentric study (EMOSIDD) is aimed at evaluatong the morphologic and electrophysiological substrate markers of increased arrhythmic risk in patients with dilated cardiomyopathy undergoing ICD implantation for the primary prevention of sudden cardiac death. We also aim to identify whether there is any electrophysiological substrate modification at the time of the first arrhythmic event in these patients. We will prospectively correlate electroanatomic mapping and cardiac magnetic resonance findings with arrhythmic events, in order to identify substrate markers of increased arrhythmic risk in patients with dilated cardiomyopathy, who are therefore more likely to benefit from a ICD implantation. In addition, electroanatomic mapping will be repeated at the time of the first arrhythmic event and compared with that one at baseline, in order to evaluate any electrophysiological substrate changes. Reduction of exposure to ionizing radiation. Radiofrequency catheter ablation is the mainstay of therapy for supraventricular tachyarrhythmias (SVT). Conventional ablation techniques require the use of fluoroscopy to navigate and position catheters within the heart, thus exposing patients to ionizing radiation with an attributable life-time risk of cancer. We recently reported the feasibility and safety of non-fluoroscopic ablation of a wide range of SVTs using the EnSite NavXTM mapping system. The NO-PARTY is a multicentre, randomized controlled trial designed to test the hypothesis that radiofrequency catheter ablation of SVTs guided by the non-fluoroscopic EnSite NavXTM mapping system results in a clinically significant reduction of the exposure to ionizing radiation compared with conventional ablation techniques. The study will randomize 210 patients undergoing ablation of SVT to either a conventional technique or one guided by the non-fluoroscopic EnSite NavXTM mapping system. All SVTs except for AF and non isthmus-dependent atrial flutter are considered suitable for randomization. Other elements of care, including drug therapy, are to follow best evidence-based practice. The primary end-point is the reduction of the total radiation dose to the patient, as assessed by dose-area product (DAP). Others pre-specified end-points include reduction of the radiation dose to the operator and reduction Fig. 3 Panel (a) shows a three-view reconstruction of both right- and left-sided chambers in a 16-year-old with a left posterior accessory pathway, obtained without the help of fluoroscopy. The LAO projection shows ablation pulses (white) from inside the coronary sinus. Panel (b) shows two modified views to better illustrate ablation pulses (white) at the mitral annulus. AP antero-posterior, LAO left anterior oblique Panel A: Bipolar voltage map of the left ventricle in left anterior oblique view. Panel B: Intracardiac echo fan intersecting the low-voltage area, showing vacuolization (asterisks) and an endocardial hyperechogenic area (empty arrow) at the basis of the anterior papillary muscle. White arrows indicate a sacculated pericardial effusion. Panel C: T2-weighted MRI short-axis (top) and long-axis (bottom) views, showing focal hyperintensity at the base of the antero-lateral papillary muscle. 160 CCM — Scientific Report 2011 — Ongoing research 2012 CCM — Scientific Report 2011 — Ongoing research 2012 161 of the total procedural fluoroscopy time. Moreover, a cost-effectiveness analysis will be performed, taking into account the additional costs associated with an ablation approach guided by the non-fluoroscopic EnSite NavXTM mapping system, and the life-time estimable benefits for the patient associated with reduced exposure to ionizing radiation. Cardiac resynchronization therapy (CRT). In the setting of cardiac pacing, our research activity is mainly focused on left ventricular pacing in CRT. The advent of CRT brought great advancement to the management of HF, with significant results over morbidity and mortality. However, a reasonable percentage of patients does not benefit from this therapy. Therefore, complementary methods such as ECG, tissue Doppler echocardiogram and electroanatomic mapping try to identify parameters capable of distinguishing the best candidates for CRT and to reduce the incidence of non-response. However, the best method to locate the optimal RV and LV pacing sites in individual patients remains unclear. A potential reason for non-response to CRT may be the presence of extensive scar tissue in the region of the tip of the LV pacing lead. Pacing the LV in non-viable or scarred myocardium may result in less effective or even ineffective LV pacing and, as a consequence, failure of LV resynchronization and no response to CRT. Accordingly, in our study (SHARE-M) we try to establish an immediately available and helpful evaluation of the acute response to CRT in relation to the myocardium substrate, scar tissue, LV dyssynchrony, fixed and functional conduction blocks, based on the novel Dynamic Substrate Mapping algorithm which permits in vivo reconstruction of cardiac anatomy and assessment of the activation sequence with high spatial resolution. Pulmonary vein isolation system in the treatment of paroxysmal atrial fibrillation (REVOLUTION Study). Radiofrequency (RF) catheter ablation has provided excellent results for treating many types of supraventricular arrhythmias. The ACC/AHA/ESC AF Management Guidelines now consider catheter ablation to prevent recurrent AF a reasonable alternative to pharmacological therapy (i.e. a second treatment option) in all categories of the treatment algorithm to maintain sinus rhythm. In fact, catheter ablation techniques targeting the isolation of the PVs are now commonly used in the electrophysiology laboratory. The 2007 115±5cm USABLE LENGTH IRRIGATION PORT 64±3cm HANDPIECE CONNECTOR CONNECTOR SHAFT LOOP LUMEN WITH IRRIGATED RING ELECTRODES CCM — Scientific Report 2011 — Ongoing research 2012 Novel surround-flow irrigated catheter for ventricular tachycardia ablation. Sustained ventricular tachycardia (VT) is an important cause of mortality and morbidity in patients with ischemic dilated cardiomyopathy (DCM). Most patients have several different ventricular tachycardia indicating a complex arrhythmia substrate. Implantable cardioverter-defibrillators often can terminate most malignant ventricular episodes with success, reducing sudden death but ICD shocks reduce quality of life and ventricular tachycardia predict increased risk of death and heart failure despite effective ICD functioning. Beyond this ICD cannot change the underlying arrhythmic substrate. Catheter ablation has been shown to be useful to reduce ventricular tachycardia recurrences refractory to antiarrhythmic therapy. Patients submitted for ventricular tachycardia ablation with a previous myocardial infarction usually show cardiac failure with low ejection fraction. In these patients fluid overloading due to the use of saline irrigation during ablation with an irrigated catheter could be critical during an ablation procedure with a large 115±5cm USABLE LENGTH 64±3cm ROTATING KNOB HANDPIECE SHAFT DEFLECTABLE LUMEN DEFLECTABLE LUMEN 162 Electrode Irrigated PV Isolation System when used for the treatment of drug refractory symptomatic PAF. CURVE DEFLETION THUMB KNOB CURVE DEFLETION THUMB KNOB ROTATING KNOB IRRIGATION PORT HRS/EHRA/ ECAS consensus statement on catheter and surgical ablation states that electrical isolation of the PVs from the left atrium is “the cornerstone for most AF ablation procedures.” It is widely considered the best method to treat AF in the paroxysmal AF population. Episodes of atrial fibrillation are initiated by ectopic sites which derive in more than 90% of cases from the pulmonary veins. One or several pulmonary veins may be implicated and often in a single vein there is a multiple initiation site. The foci originate in the muscular cardiac bundles that line the pulmonary veins. These muscular extensions occupy varying proportions of the vein perimeter, ranging from one quadrant to the whole circumference. Using electrophysiology catheters their position and extent can be precisely evaluated from the electric potentials that they generate. By isolating the pulmonary veins with radiofrequency, most cases of paroxysmal AF can be corrected (episodes lasting <1 week that resolve spontaneously) and about 20% of persistent AF cases (>1 week or requiring electric shocks long standing persistent AF is excluded). The purpose of this study is to assess the safety and effectiveness of the nMARQ™Circular and nMARQ™Crescent Mapping & Ablation catheters and the workflow of the Multi- A Circular Mapping & Ablation Catheter A Crescent Mapping & Ablation Catheter LOOP LUMEN WITH IRRIGATED RING ELECTRODES CCM — Scientific Report 2011 — Ongoing research 2012 163 Cardiovascular Imaging number of RF applications and long procedure time. The new ThermoCool SF® irrigated ablation catheter TCSF (Biosense Webster, Inc., Diamond Bar, CA.) with a bi-directional technology has been designed to provide optimal flow characteristics with a porous tip that allows highly efficient cooling and requires therefore half the flow rate to deliver the same RF power. The catheter design with uniform cooling of the catheter tip without hotsposts, claims to produce consistent lesions independent of tip orientation and could be more effective requiring a shorter application time. Use of the TCSF catheter is associated with a statistically significant reduction in fluid infusion volumes during prolonged VT ablation procedures, which may benefit patients with LV dysfunction. A trend towards reduced mean RF application time per area unit might suggest improved efficacy with the TCSF catheter. The research activity is deeply integrated with the daily clinical work including echocardiographic and computed tomographic examinations. Regarding recent research projects, our main efforts are focused on: a)new methods in transthoracic and transesophageal 3D-echocardiography demonstrating advantages of 3D vs 2D-echocardiography in the evaluation of right ventricular function, mitral valve prolapse, intraoperative monitoring of cardiac surgery, left atrial function (Fig. 1-2-3). Fig. 1 164 CCM — Scientific Report 2011 — Ongoing research 2012 Fig. 2 Fig. 3 CCM — Scientific Report 2011 — Ongoing research 2012 165 Fig. 4 b)feasibility and accuracy of non-invasive evaluation of coronary arteries, stents and by pass grafting through cardiac computed tomography (Fig.4-5) c)new technical advances in radiation dose reduction in cardiac computed tomography maintaining a high accuracy in native and stented coronary arteries evaluation. d)cardiac CT and prognosis e)new bioengineering approaches to cardiac imaging computation, mainly in the field of 3D-echocardiography (Fig. 6-7-8) f)collaboration with other Units within the framework of a disease-specific multidisciplinary team including new imaging data in the evaluation of patients undergoing electrophysiological approaches, cardiac failure therapies, PCI procedures, cardiac surgery (including percutaneous/transapical aortic valve implantation, mitral clip, left atrial appendage closure). Collaboration with other Units and integrated advanced imaging techniques are well exemplified in a clinical protocol concerning mitral valve diagnostic approaches and mitral valve surgery. In this field transthoracic 3D-echocardiography is performed before surgery to better define anatomy of the valve (recent studies from our group showed a 95% accuracy). During surgery 166 CCM — Scientific Report 2011 — Ongoing research 2012 Fig. 7 Fig. 8 Fig. 5 Fig. 6 in the pre- and postoperative phases, transesophageal 3D-echocardiography further defines anatomic details and facilitates the understanding of optimal surgical planning and surgical results. In each of these steps and during the follow-up (1, 3, 6 and 12 months) 2D and 3D examinations are performed. Data on left ventricular function and 3D shape, right ventricular 3D function, mitral valve annulus (both native and postoperative prosthetic annulus) function and shape are analyzed throughout the study. New data have been published on the remodelling of the left atrium after mitral valve repair, therefore having a very complete and comprehensive definition of changes of heart chambers after a “correct early timing” of surgery (left ventricular remodelling and shape, right ventricular dimensions and function, left atrial remodelling and function). Moreover all these 3D data are not only analyzed with available software, but also with new software and methods of analysis set up thanks to novel bioengineering approaches. Another field of interest is a novel approach to the aortic valve annulus analysis and coronary arteries in patients undergoing transfemoral aortic valve implantation. In these cases, 3D TEE allows a precise assessment of several parameters including prediction of postimplantation aortic regurgitation and the evaluation of the distance between the left main coronary ostium and the aortic valve. This integrated clinical and advanced imaging protocol is applied to the several cardiovascular fields previously mentioned. A recent field of scientific interest is the new realtime 3D-echocardiographic imaging. In particular, our attention is focused on the quantification of novel 3D left ventricular shape indices, able to overcome the limitations relevant to prior 2D indices, to better follow ventricular remodelling after surgery and to study the coupling between left ventricular function and morphology. Another field of interest is the evaluation of the dynamic motion of mitral and aortic valves. By the development of specific 3D tracking algorithms, it is possible to follow the movement and deformation of the valvular annuli in the 3D space, and quantify them by innovative CCM — Scientific Report 2011 — Ongoing research 2012 167 Fig. 9 parameters. In this way, the immediate (by TEE) and mid-term (by TTE) follow-up effect of mitral valve repair with annuloplasty on the mitral and aortic valves, as well as on their coupling, can be quantified. Moreover, the unique information derived from this analysis, together with papillary muscle tips positions, are utilized to generate a realistic computational model of the mitral valve structure, customized to the patient specific characteristics, which could be useful both in the surgical planning and in the follow-up evaluation phases. Recently a new approach has been evaluated concerning the simultaneous analysis of aortic-mitral coupling in patients undergoing mitral valve repair. These research projects are carried out in the mainframe of the “Surgaid” project (www.surgaid.org ), in collaboration with the Politecnico of Milano and the University of Bologna. In the area of non invasive evaluation of native and stented coronary arteries or by pass grafting, studies 168 CCM — Scientific Report 2011 — Ongoing research 2012 Fig. 10 have been focused on the diagnostic accuracy of 64 Slice Multi Detector Computed Tomography (MDCT) and on low radiation doses (trying to reduce with new protocols the high radiation exposure). ProspectiveECG-triggering MDCT was recently introduced at Centro Cardiologico Monzino and we showed that this protocol allows an accurate detection of coronary stenosis with a low radiation dose. Moreover, diagnostic accuracy is high not only in native coronary arteries but also in stented lesions. Another area of collaboration among different Units at Centro Cardiologico Monzino concerns MDCT advances and heart failure (including new integrated techniques for electrophysiological procedures). In details, studies are focused on the very high accuracy of MDCT in the diagnosis of idiopatic vs ischemic cardiomyopathy (thus avoiding invasive coronarography), on the evaluation of the venous coronary circulation (essential in the Fig. 11 pre-procedural planning of biventricular pacing), the CARTO techniques (integrated approaches of MDCT and electrophysiological mapping facilitating navigation of catheters inside cardiac cavities). Moreover new insights into the evaluation of the aortic annulus have been published mainly related to the importance of a precise assessment of annulus size and geometry in patients undergoing transfemoral aortic valve implantation. In the field of the long term prognosis, MDCT has been studied in patients with intermediate risk of coronary artery disease and patients affected by diabetes showing the importance of the atherosclerotic burden on long term prognosis. method of acquisition and reconstruction of images of the tricuspid annulus and right ventricle. Interestingly tricuspid annulus is relatively easily evaluated through this novel MRI method and an accurate dynamic reconstruction has been shown to be feasible. (Fig. 11). Recently MRI (Fig 9-10) has been integrated in our area and, even though the Unit start-up allowed us only a 2 years experience (with more than 1000 cases per year), we have already started the evaluation of new fields of interest such as the tricuspid valve with a new CCM — Scientific Report 2011 — Ongoing research 2012 169 Clinical Research on Atherothrombosis The research activity of the Atherothrombosis Clinical Research Unit is deeply integrated with the clinical activities of the Cardiac and Vascular Surgery Units and focuses on the translational cardiovascular features of the main diseases affecting the adult: 1. coronary artery disease 2.valve disease 3.diseases of the aorta In order to improve our capabilities to study valve and aortic diseases, we have started a clinical and research project to create a Clinical and Research Center, called MALVA (Centro di alta specialità per la prevenzione, diagnosi e cura delle MALattie Valvolari ed Aortiche). The mission of this Center is to bring together a knowledgeable and experienced multidisciplinary team of cardiologists, cardiac/vascular surgeons and other cardiology, imaging and biomarkers experts to provide: • a thorough evaluation of patients using state-ofthe art diagnostic tests • on-going comprehensive care of patients affected by valve and aorta diseases • genetic screening for families of patients with genetic disorders, such as Marfan Syndrome • ongoing research and education to provide patients with high quality and innovative therapies Finally, this unit is also focused on the study of the predictors of the main complications occurring during and after adult cardiac surgical procedures. Coronary artery disease. Coronary artery disease is one of the most diffuse diseases in the western countries, and bypass surgery is the most reliable and durable therapy for the severe forms of this disease. Even if coronary bypass surgery enables the best results in the long term, patients, particularly the younger ones, are not ensured they will be free from problems related to coronary disease during their lifetime. The clinical benefit of myocardial revascularization is related to the lack of adverse cardiovascular events and to graft patency 170 CCM — Scientific Report 2011 — Ongoing research 2012 of great saphenous vein, which is nowadays the main autologous vessel used for grafting coronaries different from anterior interventricular artery. It is well known that bypasses tend to occlude over time as well as native coronaries tend to progress their disease. Unfortunately, phenomena leading to early and late complications and to graft occlusion are not fully clarified and it is not possible to explain interindividual and temporary variability of progressive stenosis rate only on the basis of classical atherosclerosis risk factors. We know that, after coronary bypass surgery, a protracted prothrombotic and a proinflammatory status ensues, and, even if a great effort to understand the physiology and pathophysiology of the response to CPB has occurred over the last 50 years and several targeted strategies using different drugs modifying CPB components or even abolishing CPB itself have been tested in order to attenuate the systemic inflammatory and prothrombotic response occurring after CABG, none of these was able to blunt effectively the whole body activation occurring after this kind of surgery. Also, the role of this whole-body response, as 330 patients were assessed for eligibility 24 declined to partecipate before d/c from the hospital after provifing informed consent 306 patients eligible for subsequent follow-up 9 not found or not reached with phone call 297 patients contacted for phone interview at follow-up 7 dead 59 declined to accept 50 not eligible 2 CT performed elsewhere 179 Patients underwent CT scan well as the role of different antithrombotic strategies, is still not well defined. In 2011 we concluded the 18 months follow-up of the BAPPY study; in this study we collected blood samples from 330 consecutive patients before and after coronary bypass surgery and followed them up clinically performing a 64-rows CT scan at 18 ± 3 months after the surgical intervention in order to document the patency of coronary bypasses and to identify possible predictors of bypass occlusion. Concerning CT-scan assessment of patency, among the 330 enrolled patients, 179 underwent assessment of graft patency, as shown in the flowchart on the page before. patency per patient (that means how many patients have perfectly patent grafts) is 135/179 (75.4%). The patency rates of the different types of grafts are the following: LIMA n=12/75 RIMA n=6/20 Radialn= 1/5 SVG n=27/303 (6.8%) (30%) (20%) (8.9%) The main features of the study population concerning coronary disease and coronary bypass grafts that were performed during surgery, are reported in theTable 1. Patients had on average 2.7 coronaries affected by coronary atherosclerosis and received an average of 2.7-2.8 grafts per patients, mainly saphenopus vein graft and left internal mammary artery. The results of 64-rows CT scan on 179 patients show an overall patency of 366/503 graft (72.7%), whereas the Table 1 VARIABLE ENROLLED (pts, n=330) FOLLOW-UP (pts, n=297) CT SCAN (pts, n = 179) Diseased coronary vessels, (n) ± SD 2.75 ± 0.52 2.74 ± 0.53 2.77 ± 0.52 Distal anastomoses, (n) ± SD 2.73 ± 0.75 2.73 ± 0.77 2.81 ± 0.74 Saphenous vein (SVG), n (%) 531 (59.0%) 481 (59.2%) 303 (60.2%) Left internal mammary artery (LIMA), n (%) 319 (35.4%) 285 (30.1%) 175 (34.8%) Right internal mammary artery (RIMA), n (%) 35 (3.9%) 33 (4.1%) 20 (4.0%) Radia artery (RA), n (%) 15 (1.7%) 12 (1.5%) 5 (1.0%) CCM — Scientific Report 2011 — Ongoing research 2012 171 The next steps will be the prosecution of the follow-up to 5 years, and the study of the biomarkers, mainly inflammatory and haemostatic, possibly associated with poor clinical outcomes and reduced graft patency at follow-up, in order to identify new predictors, molecular mechanisms and targets of unfavourable clinical outcomes. Valve disease. Nonrheumatic calcific aortic stenosis and mitral valve insufficiency are respectively the first and the second cause of valve disease requiring surgery, whereas tricuspid valve disease is less frequent and is usually associated to advanced mitral valve disease. Calcific aortic valve stenosis is the most common heart valve disease in the western world, especially in elderly people; on average, every year in Europe and in the United States around 50.000 aortic valve replacements occur due to this pathology. The prevalence of clinically significant aortic stenosis increases progressively with age, being 2% in people over 65, and more than 4% in octogenarians. It is expected to reach the widest diffusion by the year 2030, when the “baby boomers” of the sixties will reach the age of 65 or more. The behavior of aortic valve sclerosis, a milder form of aortic valve disease characterized by calcification and stiffening of the aortic valve without a transvalvular gradient, parallels the one of calcific stenosis, the prevalence being around 20-30% in patients aged over 65 years, and reaching 45-60% in octogenarians. Now it is clear that calcific aortic stenosis is not a passive, agerelated disease. Although the progression of this disease is a multi-factorial process resembling atherosclerosis, there are some important differences in the final results. In atherosclerosis the final result is plaque development 172 CCM — Scientific Report 2011 — Ongoing research 2012 and plaque instability whereas calcific aortic disease ends up with a severe calcification of the aortic valve. This suggests that calcific aortic stenosis is not a single disease process but, more likely, a common macroscopic anatomic equivalent of a series of partly related processes (inflammation, matrix remodeling, myofibrobasts metabolism, angiogenesis, oxidative stress, and haemostatsis perturbations) that ultimately leads to severe calcification of the valve. Mitral valve prolapse (MVP), an abnormal systolic protrusion of mitral valve leaflets into the left atrium, represents a common cause of severe mitral regurgitation (MR) and it often requires surgical correction, especially in people living in industrialized countries. Available data suggest that it has a prevalence of 2% to 8% among the adult population; thus, MVP is expected to occur somehow in the life course in approximately 7,2 million individuals in the United States and in over 144 million worldwide. Besides, a marked effect on its spread and severity is played by increasing age, indeed important mitral anatomical changes are found at post-mortem in approximately 5-7% of elderly people, with males showing about twice the risk of females of developing severe regurgitation when ageing. Regarding younger people, some studies show that both genders are equally affected, whereas others document a female preponderance. In most cases this disease is a primary condition characterized by a progressive myxomatous degeneration of the mitral valve leaflets and of chordae tendinae; it represents a slowly developing process which usually shows a benign course, as less than 10% of all prolapsing mitral valves progress to severe regurgitation requiring surgery during their lifetime; however, given the wide diffusion of MVP, this translates into very high costs for health organizations in the adult population, even if only a small portion of patients will eventually need surgical treatment. Although clinical features and pathophysiology of MVP have been known from several decades, limited data are available regarding biological mechanisms or biochemical perturbations possibly implicated in its progression. The multitude of the mechanisms potentially involved in aortic and mitral valve disease progression, together with the available clinical evidence, strongly suggests that there are several unknown mechanisms possibly contributing to the progression of this disease and we have been actively investigating them with several lines CCM — Scientific Report 2011 — Ongoing research 2012 173 of research. Through a combined genomic, proteomic and transcriptomic approach we are trying to identify new genes and proteins involved in this process, studying both diseased valves and plasma of patients undergoing aortic valve replacement and mitral valve repair in order to assess what are the derangements in haemostatic, inflammatory, and oxidative stress pathways before surgery and what are the changes that surgery may correct or cause in these patients. It is very interesting to note that very limited studies are available concerning the role of oxidative stress in these two most frequent valve diseases in the western countries. For this reason we have recently completed an observational study investigating whether oxidative stress, antioxidants and nitric oxide pathways differ in control subjects and in adult patients candidate to the three most common cardiac surgical procedures performed in the adults of western countries: coronary bypass surgery (CABG), aortic valve replacement for calcific nonrheumatic aortic stenosis (Aortic), or mitral valve repair for degenerative mitral insufficiency (Mitral). We have enrolled 165 consecutive patients undergoing surgery from January to May 2011 (CABG, n=63; Aortic, n=51; Mitral, n=51, respectively). In addition, thirtythree healthy subjects with cardiovascular risk factors similar to surgery patients were also studied (Controls). Candidates to cardiac surgery had increased levels of oxidative stress and reduced levels of antioxidants with respect to Controls; also, there was a trend in nitric oxide pathways impairment in surgical candidates. Concerning differences among surgical procedures, Mitral patients had impaired glutathione and nitric oxide pathways with respect to CABG and Aortic patients. Overall, the patterns of oxidative stress and NO pathway of Mitral Patients were more dissimilar from Controls than those of CABG and Aortic patients. Moreover, an additional study investigated whether oxidative stress, antioxidants and nitric oxide pathways differ between control subjects and candidates to isolated aortic valve replacement with or without coronary atheroscle-rosis has shown that candidates to isolated aortic valve replacement had increased oxidative stress, reduced antioxidant levels and more pronounced nitric oxide pathway impairment with respect to control healthy subjects with similar cardiovascular risk factors. Interestingly, there were no differences, within aortic stenosis patients, between patients with normal coronaries and patients with coronary atherosclerosis. These data are the proof of concept that valve diseases are sensibly associated with marked levels of oxidative stress; the next step will be to determine whether oxidative stress improves after surgery and whether and how other molecular mechanisms, namely inflammation and haemostasis, are also involved in these diseases. Concerning tricuspid valve disease, we are carrying out a study to ascertain whether the different repair techniques now used to correct functional tricuspid insufficiency are equivalent or not in term of early and late results. The main point of this study is to answer a simple question: we know that over time there are 174 CCM — Scientific Report 2011 — Ongoing research 2012 many different techniques for repairing a functionally insufficient tricuspid valve. These techniques can be arbitrarily categorized into two main groups as shown in the figure: Tricuspid valve repair Anular stabilization Complete Partial Rigid ring Pericardial ring Flexible ring Bex/incomplete rings NO anular stabilization Suture plasties Bicuspidization (Kay) There are techniques that warrant annular stabilization, whereas others do not. We are actually running a metaanalysis of the studies currently available in literature to see whether there are differences between these two main repairing philosophies. Aortic disease. Thoracic aortic aneurysms (TAAs) are important causes of mortality and morbidity in western countries. Overall, they represent the 15th leading cause of death in USA, and have an estimated incidence of 1 case per 10.000 persons/year, whereas the incidences for aortic dissection and aortic ruptures are both around 3 per 100,000 persons/year. The two major etiologies of TADs are, in order of importance, degenerative/ atherosclerotic and genetic; interestingly, more than 20% of patients affected by TAA has a first-degree relative CCM — Scientific Report 2011 — Ongoing research 2012 175 with the same problem; less frequently, TAAs recognize an inflammatory/infective problem or trauma as a possible cause. The main problem a physician encounter when dealing with TAAs is that the diagnosis is usually made by an imaging study done for unrelated problems; otherwise, TAAs are usually clinically silent until one of the dramatic complications (usually recognized as acute aortic syndromes, dissection, rupture, hematoma, and penetrating aortic ulcer), ensues threatening non only patient’s life in the immediate but also often prejudicing survival and quality of life at follow-up. For this reason prevention and prediction have become a very active area of research in this field; on one side, it is important to monitor and predict TAA progression in size, on the other it is essential not only to predict but also to diagnose the occurrence of complications in a timely way. Although biological testing for disease prediction has been already discussed several times on media, the role of biomarkers in TAAs is still under definition either for routine patient screening, or for periodic follow-up, or for a prompt diagnosis in emergency conditions. Actually we are reviewing the rapidly accumulating knowledge and the new trends on the role of biomarkers in the diseases of thoracic aorta, focusing on established and emerging, arbitrarily defined, biomarkers in the fields of genetics, inflammation and haemostasis, matrix remodelling, substances/cell components/ released upon cell damage, in order to identify new possible biomarkers that will be studied in patients affected both by TAAs and acute aortic syndromes. Moreover, our unit is also active in the study of the outcomes of surgical therapies for acute aortic syndromes, especially in genetically triggered aortic aneurysms. It is known that Marfan syndrome (MFS) is the most frequent inherited disorder of connective tissue, and is strongly associated to aortic dilatation, dissection and rupture; in these patients Type B dissection occurs frequently. At present It is not known whether stent grafting, which is now frequently used in type B aortic dissection and descending thoracic aneurysms in non-Marfan patients, is a valuable option in Marfans, and reports from the literature are somehow sparse and sporadic. For this reason we are performing, together with the Department of Cardiac Surgery of Bologna University and the Department of Cardiovascular Surgery, Thoracic Aortic Surgery Program of UPENN, a systematic review of studies reporting the early and late results of endovascular stent grafting in MFS patients with type B dissection in the attempt to quantify possible benefits or potential drawbacks of this approach in these patients. adult cardiac surgery, it leads to dialysis in 1% to 5%, and increases perioperative morbidity, mortality and costs. Previous papers have studied risk factors associated with the occurrence of AKI mainly focusing on factors measurable before surgery, occasionally adding a handful of perioperative factors, mainly related to transfusion requirements, bleeding or low-output syndrome. However, the occurrence of AKI after cardiac surgery is often not immediate and other factors pertaining to intraoperative, cardiopulmonary bypass (CPB) and postoperative management of the patients could be relevant. Moreover, some factors might be measurable some time before AKI occurrence and, more importantly, could suggest appropriate strategies to prevent or limit AKI. We have recently performed a study in order to investigate: 1) what are risk factors for AKI, expanding to other perioperative variables observable before AKI; 2) whether the expansion to new variables —related to intraoperative, CPB and postoperative management of the patients — improves our ability to predict AKI. To do that, we have studied 3219 patients operated from January 2006 to December 2009. Patient preoperative characteristics, as well as intraoperative, CPB and postoperative management variables were evaluated for association with AKI with different statistical models, first including only preoperative variables followed by the sequential addition of intraoperative, CPB and postoperative management variables, and ROC analysis was used to evaluate and compare models’ discriminatory power. AKI occurred in 288/3219 patients (8.8%). Multivariable analysis identified 15 predictors of AKI; four of them were preoperative (age, diabetes, smoking and serum creatinine), four intraoperative (inotropes, erythrocytes transfusion, crossclamp time and need of a new pump run), two CPB-related (urine output and furosemide administration during CPB) and five postoperative (erythrocytes transfusion, administration of vasoconstrictors, inotropes, diuretics and antiarrhythmics). Model-discrimination performance improved from an area under the curve of 0.830 (95% CI 0.807-0.854) for the model including only preoperative variables to an area under the curve of 0.904 (95% CI 0.886-0.921) for the model including all variables (p<0.001). Our study documented that several factors influence AKI development after cardiac surgery and perioperative patients management significantly affects AKI occurrence. Predictive models can be sensibly improved by the addition of these variables, and this will be the basis for substantial changes in our clinical practice, following, as always, the postulates of translational surgical cardiovascular research. Predictors of the main complications occurring during and after adult cardiac surgical procedures. Perioperative acute kidney injury (AKI) complicates 1% to 30% of 176 CCM — Scientific Report 2011 — Ongoing research 2012 CCM — Scientific Report 2011 — Ongoing research 2012 177 Transcatheter aortic valve implant (TAVI) Prolonged life expectancy has resulted in an aging population and, consequently, in an increased number of patients with degenerative calcific aortic stenosis. Surgical aortic valve replacement (AVR) is the treatment of choice for a vast majority of patients and it is one of the most effective, well-known and 50 years old surgical procedure, offering symptomatic relief and improving long-term survival. Nevertheless, the surgical approach is associated with substantial operative mortality rates in high-risk patients. Consequently, surgery is not offered to almost one-third of patients with severe aortic stenosis owing to a combination of reasons such as advanced age, impaired left ventricular function, re-do procedure, or multiple comorbidities. Moreover, as longevity within the general population is increasing, the proportion of aortic stenosis patients with contraindications for surgery is also expected to increase. Given the limited therapeutic options in this subset of patients, there has been interest in the development of alternative, minimally invasive techniques. TAVI has less than 10 years since first in man implantation and less than 5 years in a real post-commercial setting. TAVI has rapidly become a valuable alternative to surgery and medical therapy in high–risk patients with a transfemoral (TF) or transapical (TA) approach, in case of narrow, kinked, diseased aortic and/or iliac arteries (PARTNER Trial). This innovative procedure eliminates some of the main risks associated with conventional surgical aortic valve replacement, such as median sternotomy and the need of cardiopulmonary bypass, thus opening new perspectives for those patients currently excluded from surgical practice due to advanced age and/ or the presence of concomitant diseases. TF-TAVI is less invasive than TA implant, because it can be carried out under local anaesthesia, with a small groin incision or total percutaneous approach and it does not require chest incision. With the last delivery systems, the precision of TF-TAVI is equal to the TA-TAVI, the risk of vascular complications is mitigated and the number of TFTAVI has increased more and more. 178 CCM — Scientific Report 2011 — Ongoing research 2012 Patients’ selection and access choice for TAVI is based on a preoperative multidisciplinary team approach and this procedure has to be always executed in an hybrid operative room (multifunctional operating room with fixed ceiling-mounted angiography equipment. Fig 1) by a specialized TAVI team. In the Cardiac Surgery Unit of Centro Cardiologico Monzino Hospital, TAVI program started in March 2008 with Edwards Sapien device via TA or TF approach and TAVI team is composed by a small group of cardiovascular surgeons, interventional cardiologists, non invasive imaging cardiologists (TT and TEE echocardiography), anaesthesists and nurses. In December 2011, 2 Corevalve devices have been successfully implanted via TF approach. From March 2008 to December 2011 289 patients underwent TAVI procedures (TF 195, TA 94); preoperative logistic EuroScore was 20.6 ± 11.7%, procedure success was 98.8% with 3 cases of intraoperative death and 30day mortality was 3.1% (Fig.2). Echocardiographic assessment revealed an excellent hemodynamic function of the prostheses with a physiologic mean aortic gradient and a significantly improved effective orifice area at discharge and at one month follow-up; patients improved of one NYHA class at least at one month follow-up. Transcatheter aortic valve implantation makes possible to quickly perform heart valve replacement in the clinic and with shorter recovery time, thus reducing dramatically the costs to ensure proper treatment to the population. The Unit is involved in the multicenter European SOURCE and SOURCE XT registries of transcatheter aortic valve implantation using the Edwards Sapien and Edward Sapien XT valves. Finally, the further diameter reduction of the introducer (expandable introducer) has allowed minimally invasive percutaneous technique in patients previously not eligible for the transfemoral approach due to bad vascular Fig 1 Multifunctional operating room anatomy; the availability of the Edwards Sapien 29 mm transapical and now transfemoral model has allowed TAVI treatment in patients previously inoperable due to excessive size of the native valve. Seminars and teaching courses are currently held at Centro Cardiologico Monzino with the aim to promote the technique of TAVI for severe and symptomatic aortic stenosis in high-risk patients and to develop a new figure of cardiovascular surgeon, able to employ these new technologies and techniques to offer the best range of therapeutic options for aortic stenosis patients. Due to the complexity of the procedure and the rapid rate at which the technology is evolving, TAVI team has to be the meeting point between cardiovascular surgeons and cardiologists for a collaborative effort to establish a successful program for these high risk patients. Fig 2 A TAVI delivered by TF approach CCM — Scientific Report 2011 — Ongoing research 2012 179 Arrhythmia surgery Conventional treatment of atrial and ventricular tachyarrhythmias is usually endovascular performed. There is, however, a part of these arrhythmias that does not respond to this approach; in case of ventricular arrhythmias, this may lead to patient’s death. We have been exploring the feasibility and developing new minimally invasive and standard approaches to surgically treat refractory atrial and ventricular arrhythmias in order to offer this potentially life-saving treatment to a wider patient population. Arrhytmia surgery. The treatment of heart rhythm disorders has gone through significant changes. Initially it was mainly limited to pharmacologic therapy and the transformation and adaptation of surgical procedures to a minimally invasive catheter-based approach, and subsequent hybridization of the approach, has led to a newly recognized interest in the development of surgical approaches in this field, also taking advantage from the introduction of radiofrequency energy as an ablative energy source. Presently two main fields are under development: surgical treatment of atrial fibrillation (AF) and of ventricular tachyarrhythmias. Atrial fibrillation. The prevalence of AF is 2% in the general population and approximately 10% in patients over 60 years, being the most common form of sustained cardiac arrhythmia. The incidence of AF, however, may be substantially higher, due to undetected asymptomatic AF or undersampling in patients with paroxysmal AF. With the increasing age of the population, there is no question that the prevalence will continue to rise. AF is undoubtedly a costly public health issue. Unfortunately, the actual numeric data on the economic burden of AF are sparse compared to those on other significant cardiac disease states such as stroke and congestive heart failure. Although AF is often considered an innocuous arrhythmia, it is associated with serious morbidity and mortality due to its three detrimental sequelae: 180 CCM — Scientific Report 2011 — Ongoing research 2012 1. palpitations, resulting in patient discomfort and anxiety; 2.loss of synchronous atrioventricular (AV) contraction, which compromises cardiac haemodynamics, resulting in varying degrees of ventricular dysfunction or congestive heart failure; 3.stasis of blood flow in the left atrium, which increases the risk of thromboembolism and stroke Atrial fibrillation consists of multiple re-entrant circuits within the atrium; around the vena cava, pulmonary veins, and appendages; and around areas of functional block. Creation of multiple lines of block between these non-conducting structures may prevent propagation of arrhythmic circuits. The currently available surgical ablation systems offer a wide variety of options for surgical ablation as a concomitant or stand alone atrial fibrillation procedure. Saline-irrigated radiofrequency monopolar and bipolar energy is used to produce electrically isolating lines in the atrial tissue. Two groups of patients are eligible for this type of treatment: • patients undergoing other cardiac surgery (with the prevalence of mitral valve disease); • patients with atrial fibrillation refractory to pharmacological therapy, electric cardioversion or EPS treatment Patients in the first group are always treated concomitantly for valve or, less frequently, for coronary disease requiring surgery. Bipolar and monopolar probes are used and lesions set is discussed with EP (Fig 1) according to clinical status, AF duration, left atrium dimensions, left ventricular function. Left atrial appendage exclusion is always performed. Patients of the second group are under investigation to develop a minimally invasive surgical treatment with single or bilateral minithoracothomy in order to isolate pulmonary veins and to exclude left atrial appendage, allowing less discomfort and fast recovery. For better follow-up AF recurrence is monitored with loop Fig 1 recorder and we offer muldisciplinar ambulatory control. Ventricular tachiarrhytmias. Ventricular tachycardia (VT) is a life-threatening arrhythmia that is common to all forms of heart disease and is an important cause of sudden death. The number of patients with cardiac arrhythmias is nowadays higher and higher due to people increasing age along to occurrence of hypertension, diabetes mellitus, metabolic syndrome and ischemic heart diseases. Primary prevention of ventricular arrhythmias is usually done with the aid of implantable cardioverter defibrillators (ICD), and it is well known that the use of these devices in selected patients may improve patient survival. In addition, for patients with frequent occurrences of ventricular tachycardia (VT), catheter mapping and radiofrequency ablation is available, although technically challenging. There are several factors limiting the role of catheter ablation of ischemic VT. The hemodynamic instability of patients with coronary artery disease and depressed left ventricular function limits mapping during the tachycardia. A patient may have multiple re-entrant circuits. The VT re-entrant circuits involve scarred myocardium or can be epicardial as locations that may be out of reach for RF energy to penetrate. Finally, short-term success may be eclipsed by development of new VTs with further myocardial injury. This approach controls VT in most of patients but for those with recurring VT after catheter ablation, surgery is the only available option. This is particularly true nowadays due to an emerging population of patients with new clinical characteristics, CCM — Scientific Report 2011 — Ongoing research 2012 181 In our experience we treat 19 patients (17M-2F, mean age 64.11 ± 9.7) presenting advanced forms of heart disease (mainly ischemic dilated cardiomyopathy) and malignant ventricular arrhythmias (complex arrhythmia pattern). We are now exploring the feasibility of the development of new minimally invasive and standard approaches to surgically treat refractory ventricular tachyarrhythmias in order to offer this potentially life-saving treatment to a wider patient population. An innovative surgical approach is under development for these patients, when transcatheter ablation (with endocardial and epicardial approach) has not been effective or when it is not indicated. In our multifunctional operating room we perform an electroanatomical map of the epicardial and endocardial surface with CARTO system; this allows a precise location of the areas that need to be treated in order to eliminate VT. We also do pacemapping inside the pathological area to evaluate the presence of re-entry circuits. Then the linear ablation strategy is carried out to cross the channels and connect scar areas with anatomical structure, ablation of zone with late potentials. We use cryoenergy to freeze tissues with a cryoprobe which destroys the arrhytmogenic tissue while maintaining structural integrity. Death: 3 patients • HF + MOF (after 2 months) • no VT recurrence Heart failure (after 6 months) Superimposed endo-epi voltage maps of LV showing conducting channel within lateral basal portion of LV epicardium. Arrows point to concealed entrainment site and VT termination site 182 CCM — Scientific Report 2011 — Ongoing research 2012 CCM — Scientific Report 2011 — Ongoing research 2012 183 Vascular Surgery The scientific activity of the Vascular Surgery Unit is strictly linked to the clinical activity. The Unit supports a broad range of both clinical and basic research programs in order to improve diagnosis, treatment, and prevention of diseases involving the vascular system. The Vascular Surgery Unit scientific activity is focused on six major areas: Proteomics of atherosclerotic plaques Proteomics of atherosclerotic carotid artery plaques. By applying proteomics to human carotid artery plaque extracts, we have identified a panel of proteins that are differently represented in stable or unstable plaques, thus providing an additional mean for analyzing the molecular process involved in plaque destabilization in vivo. Western blotting was used to confirm different levels of selected proteins in plaque extracts. Evaluation of low molecular mass thiol content in carotid atherosclerotic plaques. Recently several methods for thiol determination in different sample types investigating intraplaque thiols and the relationship existing between plasma and plaque thiol levels obtained from patients undergoing carotid endarterectomy, have been developed. Moreover, the amounts of intraplaque thiols bound to proteins and their correlation with total intraplaque thiols has been analyzed. Our results have shown that increased levels of intraplaque glutathione may induce important effects on plaque fate by perturbing the normal low molecular weight of thiol redox state. Oxidative stress and carotid artery stenosis and treatment Evaluation of oxidative stress in patients with carotid artery stenosis that underwent surgical carotid endarterectomy or carotid angioplasty. The oxidative stress parameters in carotid artery stenosis and the relation between oxidative stress markers and carotid artery surgical or endovascular treatments have been evaluated. 184 CCM — Scientific Report 2011 — Ongoing research 2012 Oxidants and antioxidants possible role in pathogenesis of calcific aortic valve stenosis. Previous epidemiological studies have shown that the aortic sclerotic process shares risk factors and pathogenetic similarities with atherosclerosis, in particular a common event in both conditions is the oxidative stress. Evidences indicate that oxidized low density lipoprotein (LDL) are present both in isolated cardiac valves and in atherosclerotic plaques. The role of oxidative stress is not yet well defined and clear, but it is now recognized to be a prominent feature of many acute and chronic diseases, and even of the normal aging process. In particular there are very few information about the role of oxidative damage towards lipids and proteins in heart valvular disease, because it is difficult and not even clearly defined how to assess the presence of oxidative stress. Another important area of study is “antioxidant systems” that are part of the natural defences of the human body towards oxidative stress. We are evaluating the markers of physiological antioxidant systems - free and total malondialdehyde (MDA), hydroperoxides, products of the advanced oxidation of proteins (AOPP), reduced glutathione (GSH) and glutathione disulfide (GSSG)- and markers of oxidative stress (the two main isophorms of vitamine E, α and γ tocopherol). The preliminary results have shown that oxidants and antioxidants seem to play a key role in the pathogenesis of calcific aortic stenosis; further studies are essential to better define their roles and to elaborate new and innovative therapeutic and preventive strategies. Glycosaminoglycans and cardiovascular cellular matrix The extracellular matrix (ECM) of heart valve consists predominantly of fibrillar collagens, elastic fibers, glycoproteins, proteoglycans (PGs) and complex polysaccharides, glycosaminoglycans (GAGs). ECM and GAGs are fundamental to maintain the mechanical and functional properties of heart valves and represent an active, dynamic compartment capable of providing instructional signals to adjacent cells, determining many cellular functions. A wide variety of GAGs exert considerable and variable control over the physical and mechanical properties of ECM. As a consequence, the fine structure of GAGs changes during certain diseases involve changes in the relative and/or total amounts of GAGs. In particular, modifications of the relative percentage of single polysaccharides, e.g. the ratio of Condroitin Sulfate / Dermatan Sulfate (CS/DS) that are uronic acids and of 4-sulfated disaccharides to 6- and non-sulfated disaccharides of galactosaminoglycans, and the overall charge density may occur. Therefore, CS/DS analysis, which identifies structural variations due to differential expression of the corresponding proteins responsible for their biosynthesis, may reflect tissue or cell status. The research carried out in collaboration with the School of Biosciences and Biotechnologies, University of Modena, is focused on GAG determination in normal and pathological heart valves and vein vessels. In particular the composition of aortic valves, both normal and stenotic or with insufficiency, and of mitral insufficiency in terms of GAGs is measured. Preliminary results indicate changes in the relative amount and distribution of GAGs in the posterior leaflets of mitral valves in patients suffering from mitral regurgitation. Similar data have been obtained in aortic valve degenerative disease with a decrease in the tension to which these tissues are subjected and with an abnormal matrix microstructure capable of influencing the hydration and of conditioning the mechanical weakness of these pathological tissues. As we know, the vein insufficiency represents the most common cause of lower leg swelling, affecting up to 2% of the entire population, and up to 20% of elderly people. Thus we have performed specific studies in order to assess the GAG content of saphenous veins before and after oral administration to patients of specific of glycosaminoglycans. Preliminary data indicate that the content of GAGs in pathological vein is lower than the one of normal veins. Oral GAGs administration helps to maintain the mechanical vein characteristics. Tissue engineered heart valve Heart valve substitutes, both mechanical and bioprosthetic, currently in use are unable to grow, repair or remodel within an individual. This represents a major problem for children needing valve replacement because they have to undergo multiple major surgical procedures as they grow or get older with fast-increasing mortality risks. Tissue-Engineered Heart Valves (TEHVs) represent the ideal heart valve to be replaced since they have the potential to grow and repair within the host, to minimize inflammatory and immunological responses and to limit thromboembolism. In fact, viable cells included in TEHVs can theoretically adapt to a growing and changing environment just as a native biological structure does. The aim of the project is to develop TEHVs from natural and synthetic tissue sources using an acellular biomatrix (homograft valve and polymers) as a scaffold and seeding it with viable autologous (recipient’s) cells through the following steps: 1. Biological/synthetic scaffold creation. These activities concern the decellularisation method of cryopreserved aortic valves. Valvular tissues, taken from a donor and clinically unsuitable for transplants, are processed according to the EATB cryopreservation protocols to obtain a scaffold. We are studying the possibility to develop a biopolimeric scaffold. 2.Culture and expansion of the seeding cells. Innovative dynamic culture systems (bioreactors) have been developed for this purpose in the last year. These are also fundamental for the sowing and growing of cells on the scaffold. 3.Valves recellularisation. The bioreactors CCM — Scientific Report 2011 — Ongoing research 2012 185 mechanically stimulate the scaffold and foster a proper cellular differentiation (together with different growth factors) and a correct tissue remodeling, the valves are repopulated with recipient cells. 4.Animal tests and in humans valve implants. During the lifecycle of the project, TEHVs will be tested with test rigs (stand test), animals (sheep) and finally implanted in humans for a full clinical trial. Evolution from one type of test to the other will require full clearance of TEHVs through previous method to limit animal sufferance and sacrifice, and risks for humans. At present time we are evaluating different homograft decellularization and recellularization techniques. Moreover, in cooperation with the Bioengineering Department, Politecnico of Milano, we have created a bioreactor able to mimic the human blood flow in order to test the functioning of different valves. thickness, myocardial infarction and stroke as well as congestive heart failure. The presence of vascular disease and its possible association with 25-hydroxyvitamin D levels has been evaluated using a a Doppler ultrasound. Basic and Translational Research Gene expression of molecules involved in atherosclerotic aneurismatic aortic wall perivascular fat and also in abdominal visceral to subcutaneous abdominal fat process. The aim of this project is to study the patterns of gene expression involved in inflammation, angiogenesis, cellular proliferation, thrombosis and fibrinolisis, vascular calcification and remodelling in the perivascular fat. Patient abdominal fat samples are compared with perivascular aneurysm samples fat obtained during surgical abdominal aneurysms treatment. Evaluation of vascular peripheral ultrasound disease and vitamin D levels. Vitamin D deficiency has often been associated with cardiovascular disease risk factors such as hypertension and diabetes mellitus, with markers of subclinical atherosclerosis such as intima-media 186 CCM — Scientific Report 2011 — Ongoing research 2012 CCM — Scientific Report 2011 — Ongoing research 2012 187 188 CCM — Scientific Report 2011 — Ongoing research 2012 Our data indicate that DES-treated patients show a prothrombotic phenotype both during DAT and after clopidogrel suspension. Indeed, in DES-treated patients, despite five months of DAT, the percentages of TF positive-platelets and -MPA were markedly higher as compared to those of MT patients and remained significantly higher also when patients were on aspirin only. At clopidogrel suspension, the percentage of PAC1 positive platelets, which was, during DAT, comparable to that found in MT patients, significantly increased too, further highlighting a platelet activated phenotype. Values, evaluated during DAT, of platelet–associated TF delta stimulation or F1+2 plasma levels above the median (296% and 199 pMol/L, respectively) were significant predictors of need for reintervention in the four-year follow up. Therefore, in DES patients the evaluation during DAT of parameters related to blood coagulation such as platelet-associated TF delta stimulation and F1+2 plasma levels may assist in the identification of patients who are at greatest risk of future coronary interventions. p < 0.001 p = 0.004 p = 0.002 p = 0.0001 p = 0.0005 TF Positiv e platelets (%) p = 0.006 p = 0.05 DAT ADP STIMULATED 1 month 6 months Medicallytreated ASA only patients DAT 1 month 6 months Medicallytreated ASA only patients DES-treated patients DES-treated patients Figure 2. The risk score, obtained combining values of platelet-associated TF and of F1+2, was highly associated with adverse events (p=0.0001 by log-rank test; HR 7.5, 95% C.I. 2.2-25.1, p=0.001, for one-step score increase). The area under the ROC curve is 0.82 (95% C.I. 0.65-0.98, p<0.0001), indicating a very good prognostic value. ROC Curve for Model Area Under the Curve = 0,8182 Both below the median One of the two above the medium Sensitivity Up to a decade ago the role of activated platelets in atherosclerosis was believed to be confined to thrombus formation, responsible for the clinical manifestation of the disease. More recent studies, however, emphasize that activated platelets express molecules contributing also to the onset and evolution of atherosclerotic plaque and of vascular restenosis. We recently reported the finding that platelet reactivity to classical agonists results in expression, on the platelet surface, of functionally active tissue factor (TF), the key activator of blood coagulation and protein also involved in a wide range of biological processes including induction of pro-inflammatory response and proliferation of vascular smooth muscle cells. Moreover, we also provided evidence that a significantly greater number of TFpositive platelets, with an higher thrombin generation capacity, is present in acute coronary syndrome (ACS) patients compared to either stable angina patients or healthy subjects providing a further explanation of the increased prothrombotic potential characteristic of these patients. No data are available on the behaviour of plateletassociated TF in patients treated with DES. Thus, we sought to assess it together with other platelet activation markers such as P-selectin, activated GpIIbIIIa expression as well as the number of total and TF-positive monocyte-platelet aggregates (MPA) by whole-blood flow cytometry in DES-treated patients during DAT and at one and six months after clopidogrel suspension. In order to have reference values of platelet activation in coronary artery disease (CAD), the same markers were also assessed in 40 medically-treated stable angina patients (MT). Finally we evaluated whether elevated levels of platelet activation markers in stent-treated patients, if any, may predict the risk of future revascularization in a four-year follow-up. RESTING TF Positiv e platelets (%) Drug-eluting stent (DES) implantation is the treatment of choice for patients with symptomatic coronary artery disease undergoing percutaneous coronary intervention (PCI). By reducing the rates of late lumen loss and restenosis, DES have expanded the indications for PCI into more complex anatomic subsets (long lesions, small arteries, bifurcations) in high-risk patients (renal failure, diabetes). A low rate of in-stent restenosis (ISR) after DES, however, still exists and since the population treated with DES is large, its prevalence is not negligible. DES implantation causes a massive platelet activation and dual antiplatelet therapy (DAT) with aspirin and clopidogrel for 6-12 months is the standard of care for PCI-treated patients. It is worth mentioning, on this regard, that the length of DAT is empirically set, since no study has so far assessed platelet activation at clopidogrel suspension. Figure 1. The percentage of TF positive resting platelets measured by whole-blood flow cytometry in DES-treated patients during DAT was 3 fold higher than that observed in MT patients; it further increased one month after clopidogrel suspension, and even more six months after clopidogrel suspension. After in vitro blood challenging with ADP, the percentage of TF positive platelets markedly increased (~3-4 fold delta stimulation) with respect to the unstimulated blood sample at all time points. Particularly, despite the DAT, the percentage of TF positive platelets was comparable to that found in MT patients who are in aspirin only. At clopidogrel suspension, ADP stimulation resulted in a number of TF-positive platelets significantly higher than that found during DAT, as expected, and that in MT patients. Event-free survival Prospective evaluation of platelet activation markers in patients treated with drug-eluting stents: platelet-associated Tissue Factor predicts the risk of future revascularization in a pilot study. Risk score: Plat-TF+F1+2 Both above the median Follow up (Months) 1 - Specificity CCM — Scientific Report 2011 — Ongoing research 2012 189 Proteomics-based development of biomarkers in cardiovascular disease Understanding cardiovascular diseases and their modifications requires clarification of mechanistic changes in organ phenotype over time, the influence of genetic variations, and the effects of pharmacologic, surgical, and interventional treatments. These requirements have been addressed by genetic and biochemical approaches, but a more meaningful understanding of gene expression can be achieved through characterization of the products of that expression, proteins, the essential biological determinants of disease phenotype. The ultimate phenotype of cells, organs, and organisms is reflected in the instantaneous global protein profile, the proteome; similarly, changes in human health are the result of changes in the proteomes of individual patients over time in response to endogenous and/or external stimuli. The advent of novel proteomic approaches to investigate the complexity of human illness promises to shed new light on the pathogenesis of a broad range of cardiovascular diseases. These inferences are multifaceted and include the commonly recognized role of proteomics in characterizing biomarkers and biosignatures for the prognosis and diagnosis of disease, the capability of these technologies of revealing information regarding functional subproteomes of organelles and networks in the heart and vasculature, and the importance of proteomics in defining changes in these functional subproteomes to guide future therapy. By properly applying proteomics, at least three different types of biomarkers can be potentially developed for cardiovascular medicine: mechanistic markers, clinical disease markers, and therapeutic markers. Firstly, changes in the subcellular phenotype (subproteome) of the organism can lead to alterations in proteins detectable as mechanistic markers. These changes closely reflect what is going on in the cell and how the signaling pathways are manipulated. Secondly, the arrival of the disease carries changes in proteins that are detected by proteomics, the so-called clinical 190 CCM — Scientific Report 2011 — Ongoing research 2012 disease markers. These markers are specific of the individual disease state and can indicate the state of progression, severity, and location of the syndrome. Lastly, therapeutic markers are those that become evident as the treatment of a chronic disease progresses in the patient. These markers are influenced by many factors, including individual nature of the disease, drug treatment, patient activities, etc. Under ideal circumstances, a combination of markers from these different groups would be used for a more accurate diagnosis and treatment. Despite these promising expectations, proteomics is inherently challenging because of the complexity of the molecules with which it deals, proteins, the main working parts of biological systems. Their multiple functional roles require them to be made, modified, and often quickly remodified under the control of numerous multilevel systems. Clinical proteomics is further complicated by the fact that proteins can reflect genetic differences among patients at both the structural and quantitative levels. Compared with nucleic acids, proteins show much wider variations in physical properties (which leads to greater difficulties in global separation and detection) and in abundance (protein concentrations vary by more than 1010 in plasma, which generates additional technical challenges for detection of minor components). Despite these difficulties, proteins offer the best general picture of what is working in a cell or tissue, and what is not. Thus, although proteomics is currently far from comprehensive, it can point to numerous proteins with intriguing, even if unproven, clinical utility. Furthermore, improvements in proteomic technologies that allow a more detailed characterization of protein gene products, coupled with carefully constructed clinical databases and sophisticated analytic techniques, will serve as an important bridge to connect our nascent appreciation of biological complexity with our ultimate goal of understanding and treating disease. Therefore, a deep understanding of early protein abnormalities associated with major diseases will result in a revolution in preventive medicine by greatly enhancing our ability to identify patients at risk and those with preclinical disease. Improved patient care through the use of protein markers is indeed a well-proven paradigm. For instance, use of new protein markers has become an integral part of clinical cardiology in the past ten years. Blood measurements of C-reactive protein, Indicative of therapeutic mechanism Used to adjust clinical treatment Therapeutic Markers Mechanistic Markers Clinical Disease Markers Reflective of disease molecular origin Suggestive of cellular therapies to modulate phenotype troponin, and B-type natriuretic peptide are becoming routine measures to determine risk, to diagnose, to prognosticate, and to guide treatment of coronary heart disease, acute coronary syndromes, and heart failure. Up to now, the study of protein markers has been focused on “candidate” protein approaches, whereas “omics” technologies allow unbiased assessment of how patterns of proteins differ in various disease states. Yet an obvious hypothesis is that definition of patterns of disease-related changes, including novel disease marker proteins, would provide substantially more useful clinical information than a single marker. Observational studies have shown that the combination of protein markers (for example, troponin and C-reactive protein) into panels can provide valuable additional information in stratifying risk in acute coronary syndromes. So far, there are only a few examples of the systematic approach to define such protein fingerprints, but these appear very promising. The use of protein mass spectra has been proposed as a powerful diagnostic tool for ovarian cancer. This, then, is the opportunity for clinical proteomics: to define patterns of proteins that provide clinically useful information about susceptibility to disease, diagnosis, prognosis, and guided therapy. Consistently with this objective, the Unit of Cardiovascular Proteomics aims at improving diagnosis and treatment of cardiovascular diseases with an approach based on two principal activities: identification of candidate disease markers from well-defined human clinical cohorts, animal studies or in vitro cell systems, and validation of protein patterns in clinical data sets. Cardiovascular proteomics can have therefore important direct ‘bedside’ applications, even if we are still in the early stages. However, a fruitful interaction with the clinical departments will enable us to test the relevance of new molecular markers for diagnostic, prognostic and therapeutic improvements, aiming at a rapid translation of basic findings to the clinical setting. CCM — Scientific Report 2011 — Ongoing research 2012 191 Red Blood Cells as a source of Nitric Oxide The endothelial dysfunction is a pathological condition frequently occurring in patients with coronary artery disease. It is associated with an impaired endothelium-dependent vasodilation, due to a decreased bioavailability of nitric oxide (NO). This mediator plays a crucial role in the regulation of vascular homeostasis, vasomotor tone and platelet aggregation. Several factors may reduce the bioavailability of NO and, among them, the increased oxidative stress, secondary or not to an inflammatory condition, is of particular importance. Oxidative stress impairs the NO synthesis and it may inactivate the produced NO by transforming it into peroxynitrate. Besides endothelial cells that are considered the major source of NO, also circulating cells (erythrocytes, platelets and monocytes) are able to synthesize NO. The production of NO by red blood cells (RBC) has been only recently recognized. Initially, these cells were considered only scavengers of NO produced by endothelial cells. In fact, NO is inactivated by a dioxygenation reaction with oxyhemoglobin (HbO2) to form methemoglobin (MetHb) and nitrate. Alternatively, it may bind the heme group of deoxygenated hemoglobin to form NO-Hb and/or the S-nitrosated derivative of HbO2, SNO-Hb, the latter probably involved in the regulation of blood flow. More recently, evidence that RBC constitutively carry an active NO synthase (NOS) has been provided. This calciumdependent enzyme, located both in RBC membrane and cytoplasm, metabolizes L-arg, with an activity well comparable to that of the endothelial enzyme. Based on this knowledge, the role of RBC in the NO metabolism has been revised. It is now accepted that RBC are not only mere passive scavengers but also “transporters” of bioactive NO forms (SNO-Hb and the oxidized form nitrite) and active contributors to vascular NO. Similarly to nitrite and SNO-Hb, NO produced by RBC participates in the regulation of blood flow and platelet function. In fact, stimulation of RBC-NOS with L-arg 192 CCM — Scientific Report 2011 — Ongoing research 2012 decreases platelet aggregation whereas its inhibition has opposite effects. NO produced by RBC acts also in an autocrine manner through the modulation of RBC deformability and their passage through the capillaries thus affecting the blood flow in the microcirculation. Under specific conditions (e.g. fall in Hb saturation by O2 or the passage in resistance capillary), erythrocytes release bioactive NO from SNO-Hb and from low molecular weight nitrosothiols. Erythrocytes are also able to release ATP, which in turn stimulates the NO synthesis by endothelial cells and platelets. In addition, it has been recently shown that large amounts of ADMA and SDMA are incorporated into erythrocyte proteins and that RBC carry other important enzymes of L-arg metabolism, i.e. L-arg degrading arginase and ADMA metabolizing dimethylarginine dimethylaminohydrolase (DDAH), and cationic amino acid transporters. Alteration of these enzymatic systems in RBC may be responsible for a decreased NO bioavailability either per se or in combination with a deficiency of L-arg or a decreased BH4 availability or an increase of reactive oxygen species. Consequently, alterations of RBC L-arg/NO metabolic pathway induced by specific conditions (e.g. inflammation and oxidative stress) in pathological processes such as atherosclerosis and cardiovascular diseases can be hypothesised. However, to date little is known about the conditions that impair NO bioavailability in this cell compartment. Studies carried out in our laboratory are aimed at defining the synthetic and metabolic profile of NO (NO metabolome) in RBC and plasma of healthy subjects and patients affected by coronary artery disease, in order to understand the effect of NO RBC-derived on vascular homeostasis. To this end, an integrated and innovative approach is used to define multiple metabolic changes caused by the pathological condition. In our laboratory this approach has been already set up: a number of substrates/metabolites involved in NO synthetic and metabolic pathways are simultaneously analyzed by an LC-MS/MS method. NO synthesis in RBC will be also assessed both in terms of NO synthase (NOS) enzyme expression (immunohistochemistry and Western blot method) and of aminoacid transporter expression and activity. A study is in progress to determine arginine targeted metabolome in RBC of patients with coronary macro and/or microvascular dysfunction The enzyme deputed to NO synthesis, RBC-NOS, will be detected by immunofluorescence in patients and in controls. CCM — Scientific Report 2011 — Ongoing research 2012 193 Heterogeneity of human macrophages in culture and in atherosclerotic plaque. Macrophages are immune cells which play a central role in atherosclerosis, the major underlying cause of cardiovascular events. They are involved in the initiation, progression and vulnerability of the atherosclerotic plaque. Like other immune cells, macrophages are not static but respond to a multitude of stimuli they receive from the microenvironments and consequently show high plasticity and heterogeneity. Macrophage functions can broadly be categorized by a series of dichotomies, for example, innate or acquired immunity, tissue destruction or repair, immigration or emigration, cholesterol accumulation or release, pro-inflammatory or anti-inflammatory activity. These functions could be carried out by distinct subpopulations of macrophages. A current simplified classification of macrophage phenotypes is the discrimination between pro-inflammatory (M1) and anti-inflammatory (M2) macrophages. Whereas M1 macrophages are induced by bacterial compounds or inflammatory cytokines and are mainly involved in the expansion of inflammation through the production of inflammatory mediators, M2 have immunoregulatory and immunosuppressive functions, and promote tissue repair and healing. A wide range of markers has been described to characterize different populations in vivo and in vitro. For identifying particular macrophage subsets, cell surface proteins are generally evaluated, but the study of one or only few related phenotypical surface markers greatly oversimplifies the macrophage phenotype in an in vivo situation. In addition M1 and M2 phenotypes are obtained upon in vitro stimulation and the paradigm of macrophage polarization is essentially based on in vitro results. Currently, there is still a great need for more extensive characterization of the different macrophage population, i.e. identifying a panel of markers and functional properties of distinct macrophage subset. Studies carried out in our laboratory are focused on the characterization of the distinct macrophage morphotypes identified in our culture conditions to delineate a profile in term of antigen expression and function. This cellular model might be adopted as a suitable model to study macrophage heterogeneity, a feature that has been disclosed in settings spanning from the inflammatory and wounding response to the atherosclerotic lesion. Also in atherosclerosis, macrophage heterogeneity is an accepted concept. However in this condition the M1/ M2 division is a very strong simplification of reality, indeed in atherosclerotic plaque, the micro-environment is very heterogeneous and macrophages do not interact with individual cytokines but with many other factors produced in an autocrine manner by other tissue and inflammatory cells. However the identification of macrophage phenotypes that promote different aspects of atherosclerotic disease may have implications for the development of therapeutic interventions and it has been suggested that promoting each of these subsets at different stages of disease may have therapeutic benefits. Model of induction of macrophage heterogeneity in atherosclerosis. Macrophage can polarise towards different phenotypes according to various stimuli present in the surrounding microenvironments. 194 CCM — Scientific Report 2011 — Ongoing research 2012 CCM — Scientific Report 2011 — Ongoing research 2012 195 Experimental Imaging of brain and heart ischemia Imaging techniques play now a pivotal role in biomedical sciences, both at clinical and basic level. Their use in clinical medicine is not limited to diagnosis, but is also addressed to the identification and understanding of the etiology and pathophysiology of many diseases and is essential for monitoring the efficacy of therapeutic approaches. Moreover, due to their non-invasiveness, high-definition and versatility, imaging techniques provide a unique opportunity for translating basic, in vivo, research into human applications. The goal of our research - pursued through an interdisciplinary application of different imaging approaches and, in particular, magnetic resonance imaging (MRI) and echography - is to move scientific discoveries, in particular those in the area of pharmacology, from the laboratory to clinical practice. Magnetic resonance imaging (MRI) for the evaluation of acute stroke and its response to therapy. Stroke is the second leading cause of death worldwide and has the most devastating consequences among vascular diseases, causing long-term neurological disability and incurring high societal and financial costs. Although during the last years the understanding of its pathophysiology has remarkably improved, stroke still remains an unmet medical need. In our laboratory, brain ischemia and identification of new pharmacological targets are studied principally in two models: 1. Permanent middle cerebral artery occlusion (pMCAO) surgically induced in rats or mice. The development of acute cerebral lesions are assessed over time in MRI longitudinal studies by using trace of apparent diffusion coefficient maps [Tr(D)] and T2-weighted. T2-map and gradient-echo images are performed to track inflammatory cells infiltration into the ischemic brain damage labelled in vivo by USPIO, a cellspecific MRI contrast agent taken up by microglia and macrophages. Recently we are setting up and validating fractional diffusion anisotropy (FA) Figure 1: MRI Unit (spectrometer 4.7 Tesla) (a).. Coronal section of rat brain visualized by MRI, Tr(D) ( b) and T2 weighted (c) images. Visualization, by immunofluorescence, of P2Y12-receptor expression (green) on microglia cells (red) in areas surrounding ischemic lesion (d and f) and in healthy tissue (e) from MCAO rats. 196 CCM — Scientific Report 2011 — Ongoing research 2012 analysis in order to visualize white matter alterations and reorganization after ischemic brain damage in rodents. 2. Spontaneously hypertensive rats stroke-prone (SHRSP). This animal model develops spontaneously a complex form of cerebrovascular pathology resembling the human disease. Characterization of molecular and cellular mechanisms underlying brain damage and assessment of pharmacological treatment aimed at the prevention of tissue ischemia have been extensively investigated by the MRI Unit. Delivery, trafficking and toxicity of engineered magnetic nanoparticles in macrophages and CNS cells in animal models of stroke. The goal of this research is to develop an efficient way to harness monocytes/macrophages to selectively transport MNPs to inflamed brain areas for the diagnosis and follow-up of inflammatory and ischemic diseases by MRI. Developing this diagnostic method is an ambitious goal that implies a significant scientific and technological effort and the integration of different scientific disciplines: physics, chemistry, and materials science at the nanometer scale. The potential of engineered MNPs as contrast agents for MRI will be assayed in vitro and validated in vivo in animal models of stroke. Pathophysiological characterization of renal disease by MRI and echography. Implementation of MRI analysis to the study of kidney focuses on: (i) characterization of the end-organ damage mechanisms occurring spontaneously in the kidney of hypertensive stroke-prone rats (SHRSP) with particular emphasis on the role of iron overload in the development of hypertensive nephropathy, (ii) investigation of the relationship between renal and cerebral damage, both spontaneously occurring in SHRSP, (iii) evaluation of the effectiveness of several renoprotective therapies evaluated by the use of specific micro-bubbles that allow the echographic evaluation of tissue perfusion. Figure 2: MRI gradient-echo coronal renal sections of a health rat (arrows, a) and a proteinuric SHRSP (arrows, b) with T2* decreased signal in the cortex, an index of iron accumulation. CCM — Scientific Report 2011 — Ongoing research 2012 197 Interactions between food and cardiovascular drugs Imaging approach to ischemic heart disease: cardiac-MRI and high-resolution echocardiography. In our laboratory, a model of cardiac infarction occluding permanently the left anterior descendent coronary artery has been set up in mice. This model has been used to elucidate functional and structural changes associated with ischemic heart disease and to evaluate novel pharmacological therapies. Characterization of the temporal evolution of the damage is possible using MRI and echocardiography. Both methods allow to have anatomical information of the whole cardiac cycle by cine imaging and functional information of the organ by the evaluation of parameters such as ejection fraction, end diastolic, end systolic and stroke volumes. Moreover cardiac-MRI allows to identify the ischemic area by contrast agents like gadolinium at the very beginning of the damage. Another field of interest is the echocardiographic and morphometric characterization of left atrium (LA) in adult mice and the evaluation of the relationships between atrium and ventricle function in acute cardiovascular conditions. Figure 3: High resolution Vevo2100 platform (a); e.cho 2D and color Doppler of mouse appendage at telediatolic and telesystolic frame (b); mouse heart morphology Sagittal four chamber view of mouse hearth with cardiac-MRI (b), echocardiography (c)., LA = left atrium, histology (d); LV = Left Ventricle, RV = Right Ventricle. Statins are compounds that reduce blood levels of LDL-cholesterol by competitively inhibiting HMG-CoA reductase activity in liver cells. This effect promotes the expression of lipoprotein receptors in hepatocytes, augmenting the uptake of atherogenic lipoproteins, thus reducing their circulating levels. Although formally labeled as lipid-lowering drugs, statins are actually anti-atherothrombotic compounds, due to their lipid effects and, putatively, to many other “pleiotropic” effects (antioxidant, antiproliferative, antinflammatory, and many others) demonstrated in vitro and sometimes in vivo. Numerous clinical studies have demonstrated the efficacy of statins to reduce cardiovascular morbidity and mortality of about 25 to 50%, in direct relationship with the baseline cardiovascular risk of the population. These studies prompted the massive use of statins in clinical practice all over the developed world for the primary and secondary prevention of atherosclerotic cardiovascular diseases in the last decade. In fact, statins are absolutely the most frequently prescribed cardiovascular drugs. Many other cardiovascular and non cardiovascular drugs have pharmacologically relevant interactions with a c Figure 1. Selected drugs that may increase risk of side effects of statins when used concomitantly CYP3A4 Inhibitors/Substrates Cyclosporine, tacrolimus Macrolides (azithromycin, clarithromycin, erythromycin) Azole antifungals (itraconazole, ketoconazole) Calcium antagonists (mibefradil, diltiazem, verapamil) Nefazodone Protease inhibitors (amprenavir, indinavir, nelfinavir, nitronavir, saquinavir) b 198 CCM — Scientific Report 2011 — Ongoing research 2012 Sildenafil Warfarin Others Digoxin Fibrates (gemfibrozil) Niacin Figure 2. Incidence and severity of muscle side effects of statins statins (Figure 1), generally leading to increased statin levels in blood and statin toxicity, mostly in liver and skeletal muscle. These side effects may be clinically expressed as hepatitis to liver failure in the former, or as myalgia, myopathy, or even life-threatening rabdomyolisis in the later (Figure 2). Concern of severe toxicity is one of the most frequent patients’ and physicians’ arguments for statin omission, suboptimal dosing and early withdrawal. Awareness of drug-drug interactions is very important to reduce this risk. Yet, recent observations show that not only drugs but also some specific foods may significantly interact with statins. Paradigmatic examples are the interactions of some fruit juices with specific statins. For example, numerous cases of muscle toxicity by grapefruit juice-statin interactions were reported, and pharmacokinetic studies demonstrated that consumption of grapefruit juice consistently increase simvastatin lactone [AUC(0-24) 3.6-fold; CMax 3.9fold] and simvastatin acid [AUC(0-24) 3.3-fold; CMax 4.3-fold] bioavailability (i.e. Lilja et al. British Journal CCM — Scientific Report 2011 — Ongoing research 2012 199 Figure 3. Examples of demonstrated interactions between nutrients and statins Grapefruit juice increases serum concentrations of atorvastatin and has no effect on pravastatin Atorvastatin acid 2.5-fold Atorvastatin lactone 3.3-fold Lilja JJ etal. Clin Pharmacol Ther 1999;66:1187 of Pharmacology 2004;58:56-60). Similar results had been obtained with lovastatin (Clin Pharmacol Ther 1998, 63:397-402). Moreover, grapefruit juice also significantly interacts with atorvastatin acid [AUC(0-72) 2.5-fold] as well as with atorvastatin lactone [AUC(0-24) 3.3-fold; CMax 2.6-fold] but not with pravastatin (Lilja et al. Clin Pharmacol and Ther 1999;66:118-27). Pravastatin, instead, showed a significant although modest interaction with a specific type of orange juice [AUC 0-240 min 1.5 fold] (Koitabashi Y et al. Life Sciences 2006;78:2852-2859). More recently, pomegranate juice, which interacts with several other drugs, was also implicated in a case of rhabdomyolysis by statins (Am J Cardiol. 2006;98:7056). (Figure 3). Herbs, which are erroneously regarded as innocuous beverages, may also affect statin pharmacokinetics. In fact, the herbal antidepressant St. John’s wort (Hypericum perforatum) decreases plasma concentrations of simvastatin (Sugimoto et al. Clin Pharmacol and Figure 4. Putative favourable green tea properties Figure 5. Kinetics design Effects of regular consumption of grapefruit juice on the pharmacokinetics of simvastatin Simvastatin acid 3.3-fold Simvastatin lactone 3.6-fold Lilja JJ etal. BritishJ Clin Pharmacol 2004;58:560 Ther 2001;70:518-524). A recent report also suggests a possible interaction of St John’s wort with rosuvastatin (Gordon RY et al.Am J Med, 122:2, 2009). Green tea is an herbal product massively consumed in Asian countries. As a consequence of the popularization of the many healthy properties attributed to green tea (Figure 4), the consumption of this typically oriental infusion has extended widely to western countries not only as herb teas but also as industrialized drinks. In a recent study from our group, we observed that consumption of three cups/day of green tea doubles the bioavailability of simvastatin. Based on this observation (Werba JP et al, Ann Intern Med. 2008;149:286-7; Figure 5) and the available information about the metabolic pathways of simvastatin and green tea, we speculate that the interaction observed may be related to a competition for mechanisms of transport and/ or metabolism between specific green tea cathechins and simvastatin. Extended pharmacokinetic interaction studies are being performed in collaboration with Prof. Shizuo Yamada (University of Shizuoka, Japan) and Prof. Hiroshi Watanabe (University of Hamamatsu, Japan). of the subjects with this response on green tea had lower total simvastatin bioavailability (lactone + acid) and higher acid/lactone ratio on water. These findings suggest that subjects with a low spontaneous drug bioavailability, presumably due to an increased activity of drug efflux pumps (MDR1), are more susceptible to the effect of green tea. Therefore, in 2011 we plan to search for MDR1 gene variants that could explain this phenotype. The identification of gene variants that affect MDR1 function may have wider implications in terms of potential drug-drug and drug-nutrient interactions. Similar studies were performed in Italy (Milan) and in Japan (Hamamatsu) to assess the consistency of the putative interaction in two ethnically different populations. Healthy male young adult volunteers (n= 12 in Italy and n=12 in Japan) have been recruited for the studies. (Fig. 5) The results obtained so far (n=12 Italians and n=7 Japanese) show a wide inter-individual variability in the effect of green tea on simvastatin kinetics. Indeed, we observed similar changes to the original case report in about one quarter of participants. Remarkably, most 200 CCM — Scientific Report 2011 — Ongoing research 2012 CCM — Scientific Report 2011 — Ongoing research 2012 201 Food-blood fatty acids and coronary heart disease Coronary heart disease (CHD) is a major cause of morbidity and mortality in Europe. There are well-established risk factors for CHD, including smoking, high blood pressure, raised total cholesterol, low HDL-cholesterol and type 2 diabetes. In terms of nutrition, a diet being high in saturated fat has been shown to be associated with the incidence of CHD, moreover, most evidence suggests that the type of fat is more important than the amount of fat. The observation that Greenland Eskimos (Inuit) have a low incidence of CHD despite a high saturated fat intake, has led the scientific and public interest to focus on the role of the various fatty acids in the prevention and treatment of disease, particularly CHD. Saturated and trans-fatty acids increase both n-6 and n-3 polyunsaturated fatty acids (PUFA) and decrease the risk of CHD. In fact, several evidences indicate that moderate doses of n-3 PUFA significantly decrease the risk of fatal CHD. Higher doses and longer duration of intervention may also protect from non-fatal CHD events. The exact mechanisms through which n-3 PUFA affect CHD are not well established but may include a decrease in fasting and postprandial triglyceride levels, a decrease in arrhythmias, modulation of platelet aggregation and decreased synthesis of pro-inflammatory agents. However, most of the knowledge about the effects of dietary fatty acids on CHD risk is based on observational cohort studies and controlled dietary experiments evaluating clinical effects of fatty acid intake. Instead, there is limited information on blood levels of fatty acids in patients with coronary heart disease in relation to the diet of these subjects. Aim of our ongoing study is to assess the differences in the fatty acid blood profile between healthy subjects and patients with overt coronary heart disease and to evaluate to what extent the fatty acid pattern is determined by dietary habits in these groups. This study started enrolment in 2008 and ended in December 2010. We recruited 179 patients with CHD (defined after coronary angiography and admitted to the hospital for Fig. 1: Blood fatty acids comparison between CHD and control. *p=0.03; **p= 0.004; # p=0.001; ## p=0.0001 202 CCM — Scientific Report 2011 — Ongoing research 2012 coronary artery bypass surgery) and 150 healthy volunteers. Blood samples were obtained by collecting a drop of whole blood from a fingertip and analysed by gas-cromatography. The analyses have been performed in collaboration with Prof.Claudio Galli from the Department of Pharmacological Sciences, University of Milan. Information on dietary habits referred to the previous year was based on a validated food-frequency questionnaire (FFQ) of European Prospective Investigation into Cancer and Nutrition (EPIC). We conducted also interviews using a structured questionnaire that include information on socio-demographic factors, smoking, physical activity, history of coronary heart disease in relatives. Also blood parameters (total cholesterol, LDL, HDL, triacylglycerols, glycemia), anthropometric variables (weight, height and BMI), waist circumference, blood pressure and heart rate were measured. The preliminary results of this study (71 patients and 55 controls) showed that patients with CHD have higher blood concentration of palmitic and stearic acid and total saturated fatty acids compared to controls; moreover, coronary patients showed lower blood levels of total PUFA, linoleic acid (the major n-6 fatty acid) and eicosapentaenoic acid (EPA, a n-3 fatty acid). In contrast, we found no significant differences between docosahexaenoic acid (DHA) and EPA+DHA between groups (fig. 1). DHA is considered a n-3 fatty acid that improves cardiovascular risk. Yet, no significant difference is observed in terms of saturated and polyunsaturated fatty acids intake between cases and controls. This discrepancy could be related to recall bias: cases reporting a desirable diet instead of actual diet, a time gap between adoption of correct diet and blood fatty acid modification or a different desaturation activity between groups. We also considered the associations between nutritional habits and blood level of fatty acids in the whole population. We observed a direct correlation between intake of fish and blood level of n-3 PUFA (fig. 2). Fig. 2: Correlation between fish dietary intake and blood fatty acids in all subject. **p<0.01, ## p=0.0001 CCM — Scientific Report 2011 — Ongoing research 2012 203 Role of the longevity genes p66sh/sirt1 in insulinresistance, diabetes and cardiovascular disease. T2DM is regarded as the advanced stage of a longlasting period of pre-diabetes, which includes impaired fasting glucose and glucose intolerance, frequently observed in patients with the metabolic syndrome. T2DM is one of the most deleterious risk factors for the cardiovascular system and its prevalence is alarmingly increasing, in parallel with the worldwide epidemic of obesity. Although polygenic determinants are probably involved in the genesis of T2DM, the subject’s life-style crucially affects the chance to develop pre-diabetes and T2DM. Indeed, a very frequent trigger of these disturbances is abnormal weight gain as a result of scarce physical activity and excessive caloric intake. Excessive fat in the body behaves as an expanded organ which secretes numerous mediators potentially involved not only in reducing insulin-sensitivity and worsening pancreatic beta-cell dysfunction but also Figure 1 in the pathogenesis of the life-threatening vascular complications of T2DM (Figure 1). Most of the deleterious effects of pre-diabetes and T2DM on health is related to the occurrence of microand macro-vascular complications in the medium-longterm. These include chronic renal disease, progressive retinopathy and polyneuropathy among the former and the consequences of coronary, cerebrovascular and peripheral atherosclerosis among the later. Hyperglycaemia per se, the hallmark of pre-diabetes and T2DM and the target of current anti-diabetic therapies, leads to an increase of functionally altered glycated proteins and to the formation of advanced glycosilated endproducts (AGEs), which have been involved in the pathogenesis of T2DM complications. Yet, recent clinical trials demonstrate that even the most modern drugs for glucose control, only lightly prevent T2DM complications, especially macro-vascular, which account for more than 70% of its mortality. This percentage clearly contrasts with the much lower cardiovascular mortality in non-diabetics (Figure 2). Therefore, other mediators need to be identified as possible therapeutic targets to reduce cardiovascular morbidity and mortality in the ever-growing population of diabetics. p66Shc is an ubiquitously expressed redox enzyme that generates mitochondrial ROS, which regulate insulin signalling. Recent basic studies using a gene knock out mice model (p66Shc -/-) led to ascribe p66Shc a patent role in determining body fat accretion and weight gain (Figure 3), susceptibility to AGE-induced renal disease (Figure 4) and susceptibility to atherosclerosis (MartinPadura I et al. Endothelium. 2008;15:276-87), the most typical consequences of T2DM. Hence, p66SHC and its related protein Sirt1, might turn into relevant targets for the prevention of obesity, T2DM and micro- and macrovascular diabetic complications in humans. Only one small study (Pagnin et al, J Clin Endocrinol Metab 2005) addressed the relationship between p66SHC and T2DM in humans, demonstrating an increased gene expression in patients with T2DM vs controls, which correlated with plasma levels of 8-isoprostanes, a marker of systemic oxidative stress (Figure 5). Therefore, more information is needed Figure 2: Causes of death in diabetics and non diabetics in western population Figure 3. p66Shc-/- prevention of obesity. Body weight curves of wild type and p66Shc-/- male mice fed standard or high-fat diets. From Berniakovich I et al. J. Biol Chem 2008 Figure 4. Serum and kidney tissue AGEs, plasma isoprostane 8-epi-PGF2α levels and renal NF κB/p65 activation in WT and p66Shc KO mice injected with mouse serum albumin or carboxymethyl-lysine. From Menini S et al. Diabetologia 2007. WT-MSA KO-MSA WT-CML KO-CML Serum AGEs (U/ml) Kidney AGEs (U/mg) Isoprostane 8-epi PGF2α (pg/ml) NFkB/p65 activation (OD) 2.74±0.60 7.78±0.99 83.63±7.06 0.153±0.021 2.36±0.41 6.14±0.49 77.29±5.09 0.135±0.035 9.94±1.06 30.11±2.53a 120.11±8.74a 0.543±0.097a 5.50±0.55a,b 12.02±1.24a,b 86.75±7.11b 0.188±0.036b a Values are means±SD; n=7 per group, except for NFkB/p65 activation (n=4) a p<0.001 in CML-treated vs the corresponding MSA-treated mice b p<0.001 in KO vs the corresponding WT mice 204 CCM — Scientific Report 2011 — Ongoing research 2012 CCM — Scientific Report 2011 — Ongoing research 2012 205 High resolution B-mode ultrasound imaging to substantiate the involvement of the p66shc/Sirt1 pathway in human obesity, insulin-resistance and T2DM and to investigate the possibility and clinical effects of modulating the expression and activity of these proteins by life-style changes or drugs. The Unit of Atherosclerosis Prevention and the Unit of Biochemistry of Oxidative Stress and Endothelial Function in Atherothrombosis of the Centro Cardiologico Monzino are involved, in collaboration with the Department of Experimental Oncology of the Istituto Europeo di Oncologia and the Department of Clinical and Experimental Medicine of the University of Padova, in a project aimed to investigate and dissect out, for the first time in humans, the relationship between the p66SHC/Sirt1 pathway and two tightly linked clinical expressions in patients with prevalent abnormalities of glucose metabolism: hyperglycemia and overweight/ obesity. The protocols have been designed with the aim to provide original clinical information about: 1) the relationship between the severity of fat accretion, insulin-resistance, expression and activity of the p66SHC/Sirt1 pathway in peripheral blood mononuclear cells (PBMC), subcutaneous and omental adipose tissue, and levels of markers of oxidative stress (Associations Study; 80 patients); 2) the effect of acute hyperglycemia on the expression and activity of the p66shc/Sirt1 pathway in PBMC and the association of its changes with variations of markers of oxidative stress (Glucose Challenge Study; 20 patients); 3) the effect of glucose control on the p66shc/Sirt1 pathway in type 1 and type 2 diabetic patients (Glucose Control Study; 40 patients); 4) the effect of a clinically significant weight-loss by life-style measures (diet and physical activity) on the expression and activity of the p66shc/Sirt1 pathway in PBMC and in subcutaneous adipose tissue (Weight Loss Study; 30 patients). Data analysis will also provide information about the possibility to utilize P66 SHC expression and activity in circulating PBMC as a marker 206 CCM — Scientific Report 2011 — Ongoing research 2012 Figure 5. Linear regression between total plasma 8-isoprostane levels and p66shc gene expression in PBMC from diabetics (r2 = 0.47; P = 0.0284). From Pagnin et al, J Clin Endocr and Metab 2005. of P66 SHC expression and activity in adipose tissues and about the influence of other specific vascular risk factors (hypercholesterolemia, hypertension, current smoking) on the expression and activity of P66SHC in PBMC and subcutaneous and intra-abdominal adipose tissue. The studies described above started enrolment of patients in June 2010. The studies are co-sponsored by the Centro Cardiologico Monzino, the University of Padova, the Istituto Europeo di Oncologia and the Ministry of Health (Ricerca Finalizzata). High resolution B-mode ultrasound of superficial arteries is one of emerging technologies with strong evidence for its value in risk detection of asymptomatic individuals. Amongst the imaging tests, this technique is the most powerful due to the wide spectrum of underlying morphological and functional abnormalities that can be detected, such as: vessels dimensions and geometry, wall thickness, luminal stenosis, occurrence and extent of atherosclerotic plaque as well as arterial functional properties. The assessment of abnormal arterial relaxation in terms of decreased brachial artery flow mediated dilation (B-FMD) or decreased arterial compliance, as measured by this technique also allows, in fact, the identification of endothelial dysfunction; the primary pathophysiologic mechanism of the disease which can be detected in the earliest stage of the disease. composition) potentially useful for predicting the likelihood of plaque rupture. One of the most important strength of high resolution ultrasound imaging lies in the fact that it allows not only the non-invasive and direct visualization of vessels lumen but also of vessel walls. Beside detection and measurement of atherosclerotic plaque, this technique allows the identification on the artery walls of two echogenic lines separated by a relatively anechoic space. In 1986 our group demonstrated for the first time that these two lines were generated by the blood-intima and media-adventitia interfaces, respectively. The distance between these two lines was defined carotid intimamedia thickness (C-IMT). B-mode ultrasound may also provide prognostic information directly related to atherothrombotic properties of vessels (calcifications and plaque CCM — Scientific Report 2011 — Ongoing research 2012 207 After about thirty years of researches both C-IMT and B-FMD, are now considered the most widely accepted non-invasive markers of sub-clinical atherosclerosis. Both these variables, in fact, have been widely used in clinical and epidemiological studies to investigate the effects of established and non-traditional vascular risk factors, as well as to investigate the association with end-organ damage in high-risk patients. Against this background, these ultrasound variables have a high potential to be included in a next future among the most important diagnostic tools available in the clinical practice not only for the early detection of atherosclerosis but also for the early recognition of patients at high risk of cardiovascular diseases. The general mission of our group is to increase the current understanding of the pathophysiology of atherosclerotic diseases with the final goal to implement strategies aimed at reducing the incidence of cardio- and cerebro-vascular events and minimizing the related morbidities. New knowledge in this field is absolutely desirable in order to create the scientific background needed to bring these ultrasonic markers, which until now have been mainly of research pertinence, in the clinical practice for both diagnosis and prevention purposes and to monitor the efficacy of pharmacological or dietary interventions. In this direction we are mainly interested in evaluating the reliability of methods used for the measurements of these ultrasonic variables and in understanding whether these surrogate markers: a) add independent information on risk or prognosis, b) account for a clinically significant proportion of the disease, c) provide good sensitivity, specificity and predictive value in the prediction of cardiovascular events. The strategy chosen to achieve these objectives is to use these markers from the earlier stages of the disease, well before the exordium of clinical manifestations. 208 CCM — Scientific Report 2011 — Ongoing research 2012 Studies performed to reach the Unit goals are aimed at: 1) investigating the role of conventional and emerging atherosclerosis risk factors on the basis of their effect on C-IMT and endothelial function, 2) improving the current capacities to identify patients at high cardiovascular risk by using imaging techniques. Researches aimed at investigating the role of conventional and emerging atherosclerosis risk factors on the basis of their effect on C-IMT and endothelial function. A large part of the risk to develop atherosclerosis is not explained by traditional risk factors. For example, it is known that conventional risk factors explain less than 30% of C-IMT variability, which suggests that other determinants, not yet considered, may exist. This underscores the importance of search for novel risk factors. Based on this rationale, we are now performing a series of projects that use C-IMT or B-FMD as surrogate markers of atherosclerosis to identify new vascular risk and protecting factors affecting the atherosclerotic process as well as to attempt to elucidate some uncertainties on the role of already identified atherosclerosis determinants. One of our interests in this field concerns the study of family aggregation of atherosclerosis. The role of family history of premature cardiovascular events (FHPCE) as an independent risk factor for atherosclerosis and for vascular events is a quite well established issue. However, it is not well known whether this role comes from genetic or environmental factors. Some authors have tried to confirm the nature of FHPCE as a risk factor for atherosclerosis by evaluating the amount of “offspring-carotid IMT variability” explained by parent’s C-IMT. These studies, however, reported contrasting results with an amount of offspring C-IMT variability explained by parent’s C-IMT ranging from 20 to 92%. In order to investigate whether these discrepancies might be related to the age of generational pairs considered (parent – offspring), we are currently evaluating the contribution of parent’s-IMT to offspring-IMT variability in young (parentage <60) and old (parent-age>75) generational pairs. The generic term “chronic-degenerative diseases” includes a number of clinical entities with different impact on quality of life and patient survival. Among these there are: the metabolic syndrome, the fatty liver disease and the autoimmunity; all expression of a chronic inflammatory state. Chronic inflammation, in turn, is an important risk factor for atherosclerosis. Greater knowledge of the individual etiological conditions could produce a significant reduction of the impact of these diseases. This raised our interest in the study of interaction among these chronic-degenerative diseases. Therefore, the Unit started a collaborative study with the Department of Medicine, Surgery and Odontoiatry , University of Milano, with the ASL Milano 1- Az Osp Legnano/ Presidio Ospedaliero di Abbiategrasso, with the Association of Hepatology (ACE) of Reggio Calabria and with National Centre for Epidemiology, Surveillance and Health Promotion, Istituto Superiore di Sanita, aimed at determining the prevalence of metabolic, inflammatory and autoimmune risk factors for early cardiovascular damage and their association with early cardiovascular damage. One of the uncertainties on the pathophysiologic role of already identified vascular risk factors concerns the relationship between high density lipoprotein cholesterol (HDL-C), enzymes involved in HDL metabolism and carotid atherosclerosis. The relationship between C-IMT and HDL-C may strongly depend on the arterial effects of the specific/prevalent molecular mechanism that determine low or high HDL-C levels. For example, the role in atherosclerosis of enzymes involved in the reverse cholesterol transport such as plasma cholesteryl ester transfer protein (CETP) and lecithin: cholesterol acyltransferase (LCAT) is still not completely defined. In the attempt to give an answer to these questions, the Unit designed a study aimed at: a) analysing in a large population the correlation between plasma levels of LCAT and CETP and C-IMT; b) analysing the correlation between plasma levels of LCAT and CETP and plasma lipid concentrations; and c) investigating whether the relationship between plasma levels of LCAT and CETP and carotid atherosclerosis is affected by different lipid concentrations. Cigarette smoking is one of the most important risk factors for atherosclerosis. Although the marked harmful effect of cigarette smoking on cardiovascular health is well established, many people continue or even start smoking. The demonstration of vascular benefits consequent on smoking cessation would encourage abandoning this habit, particularly in asymptomatic subjects, who are less motivated than patients with overt cardiovascular symptoms. In this field, we are now concluding a study designed to evaluate whether brachial flow mediated dilation (B-FMD) may be used as surrogate biomarkers of subclinical atherosclerosis to develop clinical models which may be used to deeply investigate the vascular effects of active smoking. Specifically, we are now performing studies designed to determine the effect of acute (single cigarette) and chronic use of light or heavy cigarettes on B-FMD. Studies focused on the role on subclinical atherosclerosis of other emerging vascular risk factors, such as C-Reactive Protein and other inflammation markers, and socio-economic risk factors, such as occupation, are currently ongoing. Research aimed at improving our current capacities to identify patients at high cardiovascular risk by using imaging techniques. A large number of cardiovascular events occurs in asymptomatic individuals, therefore prevention has to include not only secondary prevention in patients who survive a vascular event but also primary prevention for the early identification and treatment of patients at significant risk. This early recognition of high risk patients is extremely important since coronary heart disease is often lethal at presentation. CCM — Scientific Report 2011 — Ongoing research 2012 209 210 CCM — Scientific Report 2011 — Ongoing research 2012 Cumulative event-free rate (%) Cumulative event-free rate (%) A number of recent clinical and experimental evidences show that diagnostic possibilities may increase if vascular risk factors are managed by using a “Global Risk Assessment’ approach. In fact, provided they are included in specific mathematical algorithms, the determination of traditional risk factors such as hyperlipidaemia, hypertension, smoking, diabetes mellitus and physical inactivity, may actually represent a useful first step to identify, among asymptomatic individuals, those who could be at risk for a vascular event from those who are not. This approach, for example, allows the stratification of individuals into high, intermediate and low risk categories. Unfortunately, also using the “Global Risk Assessment” approach, our capacity to predict the cardiac risk is quite limited and does not exceed the 6065%. The result is that patients considered at intermediate risk often develop unexpected vascular events and this suggests that at least subjects at intermediate risk need to be considered as candidates for additional tests to better refine their risk estimate and to select the most appropriate intervention. The need to improve the risk prediction has prompted the search for novel markers of cardiovascular risk. Amongst these, imaging techniques have been proved to have the highest potential to improve the estimation of cardiovascular risk provided by traditional risk factors and 1.00 Panel a 0.98 1st quintile 2nd quintile 3rd quintile 0.96 4th quintile 0.94 0.92 0.90 Quintiles of IMT mean-max 0 6 12 18 5th quintile 24 30 36 Months 1.00 Panel b 0.98 1st quintile 0.96 2nd quintile 3rd quintile 0.94 0.92 0.90 4th quintile 5th quintile Quintiles of ICCAD 0 6 12 18 24 30 36 Months Kaplan-Meier event-free curves with respect to the combined end point (any cardiovascular, cerebrovascular or peripheral vascular event) according to quintiles of the IMTmean-max (panel a) and ICCAD (panel b) Cumulative event-free rate (%) The logical workup for risk assessment in primary prevention should initially be based on traditional risk factors. However, exposure to one or more cardiovascular disease (CVD) risk factors is highly prevalent also in individuals who do not develop clinical disease. On the other hand, cardiac events occur also in many individuals who have no established risk factors for atherosclerosis. The experience from epidemiological and clinical research also suggests that no single atherosclerosis risk factor possesses the necessary requirements for an accurate recognition of patients at CVD risk. Thus, the diagnostic possibilities to discriminate between individuals who are actually at risk from those who are not by using single vascular risk factors is quite limited. 1.00 0.98 Low IMT - Low ICCAD High IMT - Low ICCAD Low IMT - High ICCAD 0.96 0.94 0.92 IMT mean-max and ICCAD above below the median 0.90 0 6 12 18 24 30 High IMT - High ICCAD 36 Months Additive effect of IMTmean-max and ICCAD assessed by stratifying the study population into 4 groups according to the presence of IMTmean-max and ICCAD values above or below the median. global risk scores and to enhance the detection of the high risk or vulnerable patients. With this objective, we have recently observed that the mean-maximal value of carotid IMT (IMTmean-max) and the carotid diameter measured in plaque free areas (ICCAD) are both associated to successive vascular events in this large group of European subjects at high risk of atherosclerosis for the presence of at least three vascular risk factors. -0.16 Framingham Risk Factors (FRFs) CC-IMTmean Bif-IMTmean ICA-IMTmean CC-IMTmax Bif-IMTmax ICA-IMTmax ICCAD IMTmax IMTmean IMTmean-max ICCAD+IMTmax ICCAD+IMTmean ICCAD+IMTmean-max FRFs+CC-IMTmean FRFs+Bif-IMTmean FRFs+ICA-IMTmean FRFs+CC-IMTmax FRFs+Bif-IMTmax FRFs+ICA-IMTmax FRFs+ICCAD FRFs+IMTmax FRFs+IMTmean FRFs+IMTmean-max FRFs+ICCAD +IMT max FRFs+ICCAD +IMT mean FRFs+ICCAD +IMT mean-max -0.04 -0.02 The additive effect of these two variables in the risk stratification was evident also when the study population was stratified into four groups according to the presence of an IMTmean-max and ICCAD above or below median. In the same study we have also shown that the combination of IMTmean-max and ICCAD with vascular Risk factors can be used to enhance the predictability of cardiovascular events. -0.00 0.02 0.04 P <0.0001 <0.0001 <0.0001 <0.0001 <0.0001 <0.0001 0.0001 <0.0001 0.048 0.042 0.43 0.99 0.89 Werse reclassification 0.0001 0.0008 0.0001 0.002 0.0005 <0.0001 0.0002 <0.0001 <0.0001 <0.0001 <0.0001 <0.0001 <0.0001 Better reclassification P Bonferroni 0.0004 <0.0001 0.0004 <0.0001 <0.0001 0.0006 0.0006 0.003 0.001 0.006 0.0003 <0.0001 <0.0001 <0.0001 <0.0001 <0.0001 Integrated Discrimination Improvement (IDI) as compared to a model including only Framingham Risk Factors (age, gender, total cholesterol, HDL-cholesterol, systolic blood pressure, hypertension, diabetes and current smoking). CCM — Scientific Report 2011 — Ongoing research 2012 211 High resolution B-mode ultrasound imaging for the assessment of mechanisms involved in atherosclerosis progression 212 CCM — Scientific Report 2011 — Ongoing research 2012 recently concluded in our Institute. The main objective of this study, funded by the European Union, was to evaluate the association between carotid IMTprogression within 15 months and the rate of subsequent (from the 15th to the 36th month of follow up) vascular events in an European population of patients at high risk of cardiovascular disease. To reach the study objectives, 3703 patients have been followed for 36 months. Of these patients, 1050 have been recruited in Finland (2 clinical centers both in Kuopio), 533 in Sweden, 532 in The Netherlands, 501 in France, 1095 in Italy (2 clinical centers: Milan and Perugia). The analyses of baseline results of this study clearly showed that latitude is an important determinant of C-IMT, which is not explained by between-country differences in established vascular risk factors (Baldassarre D. et al., Eur Heart Journal. 2010; 31: 614-622). Researches aimed at understanding the molecular mechanisms involved in atherosclerosis progression. New advances in B-mode imaging technologies have led to improved quality in detecting minute changes in ultrasonic images, allowing the assessment of even microscopic changes, of carotid atherosclerotic plaque and overall of carotid intima media thickness (C-IMT). The possibility to perform these measurements with an extremely high accuracy and precision joined with the possibility to identify different C-IMT progression patterns suggests that this high ultrasonic technique may be also used to monitor the natural evolution of the atherosclerotic disease as well as to monitor the effects of antiatherosclerotic interventions. Against this background, and in view of a) its correlation with coronary atherosclerosis and b) its capacity to predict incident coronary events, C-IMT has been widely used in clinical trials, as a substitute for angiography or vascular events, to investigate the effectiveness of pharmacological and dietary interventions. Despite hundreds of studies published so far, a number of important issues related to the evolution of atherosclerosis remains to be addressed. Therefore studies specifically focused on the assessment of mechanisms involved in atherosclerosis progression are desirable. The general mission of our group in this field is to increase the current understanding on carotid atherosclerotic progression with the final goal to understand the mechanism involved in the natural evolution of the disease as well as in the changes of this evolution induced by antiatherosclerotic interventions. In this direction, besides the assessment of reliability of methods used for the measurements of C-IMT progression, the Unit is mainly interested in the recognition of determinants of C-IMT-progression and in understanding whether C-IMT progression a) may add independent information on risk or prognosis, b) provides good sensitivity, specificity and predictive value in the prediction of cardiovascular events c) may be actually used as a surrogate endpoint in place of vascular events in studies aimed at evaluating the efficacy of antiatherosclerotic intervention. 1.00 Cumulative event-free rate (%) In an epidemiological study carried out in middle-aged American adults (ARIC study), significant associations were found between C-IMT progression (9 years of follow-up) and change in LDL cholesterol, triglycerides, onset of diabetes and onset of hypertension. Interestingly, the associations between C-IMT progression and changes in risk factors over the same period were somewhat stronger than those observed with the same vascular risk factors measured at baseline. In another study (the Framingham study) investigators observed that the association of carotid atherosclerosis with time-integrated risk factor levels is stronger than with concurrently measured risk factors, thus suggesting that those factors, emerging as most important for C-IMT change analysis, may represent the current determinants of atherosclerosis progression rather than those long persisting factors that affect such progression over a lifetime. Taken together these findings suggest that while a one time measure of C-IMT probably reflects the effect of exposure to risk factors which have acted over the whole patient’s lifetime, the C-IMT progression better reflects the effect of risk factors which have acted in the period shortly preceding the scan. In fact, if an individual changes his lifestyle or his pharmacological treatment shortly before the ultrasonic scan (or perhaps even 1 to 2 years before), the C-IMT may be poorly related to concurrently measured risk factors and ultimately, to outcome. In this kind of individuals, it has been hypothesized that C-IMT-progression might be a better index of future CVD risk than any cross-sectional estimation of subclinical arterial disease. Despite all these evidences, unfortunately it is still currently unknown if this technique could provide a specific or sensitive clinical predictor of incident CVD for an individual patient; thus, studies of the ability of change in C-IMT to predict clinical events in subsets of symptomatic as well as asymptomatic individuals are needed. A multicenter, longitudinal, observational study (The IMPROVE Study) specifically designed to address this topic has been 0.99 0.98 0.97 1st tertiles 0.96 2nd tertiles 0.95 0.94 0.00 3rd tertiles Tertiles of Fastest IMT progr (P=0.005 by Log-Rank Test) 5.00 10.00 15.00 20.00 25.00 Time (Months) to event/censoring Kaplan-Meier event-free curves with respect to the combined endpoint stratified for tertiles of the Fastest-IMTprogr. In this contest we have observed that the fastest progression detected in the whole carotid tree, regardless the location in which it was occurred (Fastest-IMTprog) is the unique IMT progression variable significantly associated to successive vascular events in European subjects More than 20 years of experience in the field have conferred to the Unit the role of Coordinator and Core Laboratory in national and international multicentre studies on the epidemiology of atherosclerosis. In order to reach the Unit goals, our studies aim at: 1) understanding the molecular and environmental mechanisms involved in atherosclerosis progression, 2) investigating the possibility to interfere with this progression by using life-style and drug interventions. Research aimed at investigating the possibility to interfere with atherosclerosis progression by using lifestyle and drug interventions. There is a substantial residual risk of CVD in patients optimally treated with LDL-C lowering drugs. While LDL-C lowering remains the primary lipid therapeutic goal, evidences suggest that raising plasma levels of HDL-C and lowering triglycerides with either nicotinic acid or fibrates also reduces CVD risk (Coronary Drug Project, HHS, VA-HIT, BECAIT, etc). Although different types of novel HDL-C therapies are currently in development, nicotinic acid and fibrates still remain the only HDL-C drug therapies approved/available so far. Nicotinic acid and fibrates, however, modify HDL-C levels by different molecular mechanisms and may differently affect the functionality of HDL particles. The attention to the mechanism of HDL-C increase and to HDL particle function was recently drawn by the results of the ILLUMINATE trial, which showed a paradoxical increased risk of cardiovascular events in patients that achieved a more than 70% rise in HDL-C levels with the CETP inhibitor torcetrapib. Thus, understanding the effect of drugs not limitedly on the HDL-C level but CCM — Scientific Report 2011 — Ongoing research 2012 213 New methods to analyze complex ultrasound measures and atherosclerosis progression also on the HDL composition (or quality) and function is emerging as a critical issue for the choice of optimal HDL-modifying therapies. Therefore, the Unit aimed to assess comparatively the effects of nicotinic acid and fibrates on HDL levels, composition and functionality in patients with low (< 40 mg/dL) and normal (between 40 and 59 mg/dL) HDL-C levels in a multicenter, open, randomized, crossover study. In collaboration with the Department of Pharmacological Sciences, University of Milan, exploratory research technologies have been used to conduct these investigations, including assessment of drug effects on: a) Reverse Cholesterol Transport (RCT), as measured by the capacity of serum to promote cholesterol efflux from macrophages and hepatoma cells; b) HDL particle number, size and composition; c) Levels and activity of HDL modifying enzymes/transporters; d) Anti-oxidant, anti-inflammatory and anti-thrombotic HDL properties; e) Endothelial Function (indexed by B-FMD). Carotid Intima-Media Thickness (c-IMT) is a well accepted surrogate marker of subclinical atherosclerosis. IMT measurements can be performed at different locations in the carotid artery and with different protocols (e.g. as the average or the maximal of a series of measures taken in a specific carotid segment). In order to identify the best measure, or combination of measures, we can use, as a criterion, the optimal prediction of future cardiovascular events. To accomplish this task, however, not only sensitivity and specificity must be considered, but also feasibility and costs, in view of the large number of exams to be performed in clinical research and patients screening. Our group is engaged in a study based on two different cohorts, one of about 2000 subjects enrolled in the Milano area, and one of 3700 subjects from five Europeans countries. Both cohorts were followed-up for at least 36 months and incident cardio- and cerebrovascular events were recorded. Epidemiology of subclinical atherosclerosis: links with social class, geography and diet. A low socioeconomic status (SES) is associated with the majority of diseases, including CVD and atherosclerosis. The interest of our group has focused for a long time on the analysis of Carotid Intima-Media Thickness (c-IMT), a well accepted surrogate marker of subclinical atherosclerosis. In this study we employed the database including more than 3700 subjects from five different European countries, and we analysed the relationships between c-IMT, social class (as denoted by three job categories: manual workers/ service workers/ white collars) and geographical area (Northern Europe vs Italy). As expected, c-IMT was strongly associated with low social class, with a positive trend going from white collars to manual workers. The novel, unexpected finding was that this trend was observed only in northern Europe and completely absent in Italy (Fig.1). White collars from northern Europe had the same IMT levels as white collars in Italy, but the spread was apparent 214 CCM — Scientific Report 2011 — Ongoing research 2012 when considering service and manual workers. To be noticed that this analysis was adjusted not only for age, gender and conventional vascular risk factors, but also for education. Thus, some other factor must explain why social class is associated with c-IMT in France, Netherlands, Sweden and Finland but not in Italy. A potential explanation may be found in the different dietary patterns in the North and South of Europe. For long-time the Mediterranean diet (Med-Diet), rich in cereals, vegetables, fish, olive oil and red wine, has been thought to protect from cardiovascular disease, whereas the typical northern-Europe diet, based on meat, dairy products and saturated fatty acids, has been linked to an increased risk of atherosclerosis. In our study we observed that in northern Europe the adoption of a Med-Diet (as measured by an appropriate score) was, as expected, much lower than in Italy; however, the interesting finding was that, whereas in Italy all social classes exhibit, on average, about the same Med-Diet high SOCIAL CLASS Figure 1 Subclinical atherosclerosis and lifelong profession, in Northern Europe and in Italy CCM — Scientific Report 2011 — Ongoing research 2012 215 score, in the North there is an apparent negative trend form the highest to the lowest class (Fig 2). The reason may be that the foods typically associated to the Meddiet (e.g. pasta, olive oil, wine) are more expensive in the North than in Italy, and thus are consumed mainly by the most affluent classes. These results corroborate the hypothesis that the adoption of a Med-Diet may be a crucial factor in preventing atherosclerosis. Development of summary scores based on clusters of soluble markers of inflammation, oxidative balance and endothelial function. Oxidative stress is usually defined as an imbalance between radical oxygen species (ROS) production and antioxidant defenses, which leads to oxidative damage and dysfunction of macromolecules, cells and tissues. Our group has recently proposed the OXY-SCORE, a comprehensive index of oxidative stress, derived from a computation of different variables relevant for the oxidative balance. We have previously reported that the Figure 2 Adoption of a Mediterranean diet and lifelong profession, in Northern Europe and in Italy 216 CCM — Scientific Report 2011 — Ongoing research 2012 OXY-SCORE is more sensitive than individual oxidative markers in detecting even slight differences in oxidative status between age and gender groups in healthy subjects. In 2008 we carried out a study to compare OXY-SCORE with its individual components in a specific clinical setting characterized by significant oxidative changes. A panel of plasma markers was measured in patients subjected to coronary artery bypass graft surgery with or without utilization of cardiopulmonary bypass (CPB or OPCAB, respectively), two clinical circumstances with patent differences in the fluctuations of the oxidative balance. Plasma malondialdehyde, oxidized and reduced glutathione, individual antioxidant capacity, alpha- and gamma-tocopherol and urinary isoprostanes were measured before, during, and after surgery. OXY-SCORE was computed at each time point. The performances of the individual biomarkers and of OXY-SCORE in discriminating the two classes of patients and in assessing major and minor variations in the oxidative balance were then compared. The results indicate that the ability of OXYSCORE to correctly classify the patients is excellent, with an area under the ROC curve of 0.90 and 0.78 during and after surgery respectively. Free MDA performed slightly better in this task, but, in contrast with OXY-SCORE, it was insensitive to the minor variations of the oxidative balance in the OPCAB group. The performance of all the other individual biomarkers was definitely worse. In addition, we are planning to devise and validate a similar score based on biochemical markers associated with endothelial (dis)function and nitrogen monoxide (NO) metabolism: L-arginine; asymmetric dimethylarginine (ADMA); symmetric dimethylarginine (SDMA); tetrahydrobiopterin (BH4). New models for the analysis of familial aggregation of atherosclerosis. The association between the level of c-IMT in the probands and a reported cardiovascular disease in first degree relatives has been widely documented. Development of theoretical models of atherosclerosis progression. The aim of this project is to test different life-long models of atherosclerosis progression, as assessed by c-IMT. Specifically, we consider two competing models, one based on a steady, linear progression throughout the entire life-span, and one based on an “S” shaped growth curve, characterized by a flat stage followed by an abrupt increase and a subsequent stasis at a ‘saturation’ level. The study is based on two datasets: a subjects with a wide age range (6-90), and a dataset of longitudinal measurements (3700 subjects dataset of cross-sectional c-IMT measures taken on about 3500) that will allow computing actual progression rates. The results from the two datasets will be merged with an approach analogous to that proposed by Ware (Am J Epidemiol 1990;132) and by Xu (Am J Epidemiol 1995;141). Another important objective of this study is the analysis of the differences in the time course of c-IMT progression in men and women, in order to identify potential genetic, environmental or physiologic (such as menopause occurrence) risk modifiers. Figure3 shows the plot of c-IMT vs age in the cross-sectional dataset. Figure 4 shows the corresponding vascular mortality rates in the Italian population. Figure 3: Cross sectional IMT data in 3500 subjects age 6-90 Figure 4: Vascular mortality rates in Italy, 2002. This association is considered to be the result of both genetic and shared environmental components. We are developing statistical models to measure the differential effects depending on the kind of affected first-degree relatives (father, mother, brothers or sisters), in order to understand the pattern of disease inheritance. A database including 3711 subjects, recruited in five European countries, will provide the data for this project. The database includes, for each subject, a variety of c-IMT measures and a complete collection of information about a history of cardio-, cerebro- and peripheral vascular disease for all first-degree relatives. We are testing a model similar to that proposed by HouwingDuistermaat and Van Houwelingen (Houwing-Duistermaat JJ, Van Houwelingen HC. Stat Med 1998;17:2865) for the development of a family indicator summarizing the information available for all relatives (CVD Family Score). CCM — Scientific Report 2011 — Ongoing research 2012 217 Cardiovascular epigenetics Development of new methods to assess carotid IMT progression. Cross sectional C-IMT measurements are considered a well established marker of the advance of subclinical atherosclerosis and have been successfully employed in the prediction of future cardio/cerebro-vascular events. However, longitudinal C-IMT measurements and, specifically, the assessment of C-IMT progression have yielded to conflicting results as predictors of vascular events. A likely explanation for this inconsistency is that C-IMT progression, as computed by the traditional approach (i.e. as the change of segment-specific measurements or of summary measures, such as the overall mean or maximum IMT), is too affected by measurement error, which dilutes all potential statistical associations with vascular events. The aim of this project is to identify novel C-IMT progression variables less affected by measurement error and thus exhibiting a stronger association with vascular events. An example of such variables is the measure of the ‘fastest IMT progression’, i.e. a sharp increase of IMT occurring anywhere in the carotid tree. Interestingly, if the fastest IMT progression is proved to be the best variable to describe atherosclerosis evolution, this will imply that this phenomenon tends to be focalized, at least in a short term, in definite spots, instead of being diffused in all carotid segments (Figure 5). Improvement of statistical approaches aimed to optimize algorithms for risk prediction. Our group is engaged in a study aimed to identify the most effective procedure to integrate new variables (specifically c-IMT measures) in the existing algorithms for cardiovascular risk prediction. We are focusing on the Framingham Risk Score (FRS) and on the new ‘Cuore’ algorithm, developed by the Italian National Institute of Health. The main goal of the study is to verify whether intermediate-risk individuals (say with an FRS between 10 and 20), positioned in a sort of “grey area” between 218 CCM — Scientific Report 2011 — Ongoing research 2012 low and high risk, can be better classified by taking into account the c-IMT. An obvious benefit is that individuals reclassified as at high-risk could beneficiate of potentially life-saving treatments. The analyses are carried out on a database of about 1000 patients with a median followup of 5 years. To test the impact of new variables in the prediction of future events we are evaluating innovative approaches such as the ROC curves analysis applied to survival data (Pencina MJ. Stat Med 2004;23:2109), and methods based on the computation of reclassification indexes, such as NRI (Net Reclassification Index) or IDI (Integrated Discrimination Improvement) (Pencina MJ. Stat Med 2008;27:157–172). Figure 5: Different models for the dynamics of IMT progression Background The molecular basis of epigenetics is complex; it involves modifications of the transcriptional status of certain genes but not the basic structure of DNA. This mechanism enables differentiated cells in a multi-cellular organism to express only the genes that are necessary for their own activity whereas the others are silenced. Epigenetic changes are preserved across cell generations and, in addition to gene silencing, specific epigenetic processes include imprinting and X chromosome inactivation. There are several layers of gene expression regulation. Among them, chromatin remodeling represents a hot field of investigation. Chromatin is a polymer of nucleosomes, constituted by DNA wrapped around histones. Modifications in DNA wrapping usually correspond to gene expression changes. Chromatin remodeling depends on two main mechanisms, both ruling the differentiation of higher eukaryotes. Post-translational modification of aminoacids in histone proteins. Aminoacids in histones are usually positively charged. If histone charge changes, the shape of the histone sphere may be modified. Since DNA is not completely unwound during replication, modified histones may be carried into each new copy of the DNA in which they may act as templates. The unstructured N-termini of histones, i.e. the histone tail, can be highly modified by acetylation, methylation, ubiquitylation, phosphorylation and sumoylation. Acetylation generally correlates with transcriptional competence as it removes the positive charge, causing DNA unwinding from the nucleosome. When this occurs, complexes like SWI/SNF and other transcriptional factors can bind to the DNA, allowing RNA polymerase-dependent gene transcription. In addition, the positively charged tails of histone proteins from one nucleosome may interact with the histone proteins on a neighbouring nucleosome, causing them to pack closely. Lysine acetylation may interfere with these interactions, causing the chromatin structure to open. Lysine acetylation may also help recruit other activating chromatin modifying enzymes and basal transcription machinery as well. Methylation of histone lysines has long been associated with constitutively transcriptionally silent chromatin. However, recently it has been shown that tri-methylation of histone H3 at lysine 4 is strongly associated with and required for full transcriptional activation. It should be emphasized that the transcriptional effect of histone modifications is position-dependent. Multiple modifications may occur at the same time, working together to change nucleosome behaviour. Addition of methyl groups to the DNA. DNA methylation, mostly at CpG sites, converts cytosine to 5-methylcytosine. Basically, certain enzymes (such as DNMT1) have a higher affinity for the methylated cytosine. If this enzyme reaches a methylcytosine in one of the DNA strands, it will methylate the other. Highly methylated areas tend to be transcriptionally less active, through a mechanism not fully understood. Methylated cytosines also marks inherited parental chromosomal areas in the zygote, a phenomenon termed genetic imprinting. Because 5-methylcytosine is chemically very similar to thymidine, CpG sites are frequently mutated and become rare in the genome, except at CpG islands where they remain unmethylated. Thus these epigenetic changes have the potential to direct increased frequencies of permanent genetic mutation. Epigenetics and cardiovascular diseases Recent genetic and biochemical analyses indicate that epigenetic changes play an important role in the development of cardiac hypertrophy and heart failure; e.g. dysregulation in histone acetylation status (see figure 1) has been linked to an impaired contraction ability of cardiac myocytes. Although such epigenetic changes should eventually lead to alterations in the expression of genes associated with the affected CCM — Scientific Report 2011 — Ongoing research 2012 219 histones, little information is available on the genes responsible for the development of heart failure. Current efforts at the Centro Cardiologico Monzino have focused on deciphering the network of genes which are under abnormal epigenetic regulation in dystrophic skeletal muscle and heart. To this end, coupling chromatin immunoprecipitation to high-throughput profiling systems is being applied to endothelial, smooth muscle cells and cardiac myocytes in normal as well as in affected hearts. Further, members of different classes of histone modifying enzymes as well as high weight molecular complexes formed by chromatin modifiers are studied. Given the pivotal role of nitric oxide in the pathophysiology and epigenetics of cardiovascular cells (see figure 2), the possible involvement of a dysregulation of nitric oxide-dependent epigenetic mechanisms is currently investigated. The results of these studies should not only improve our understanding of the molecular basis of important cardiovascular alterations including hypertrophy and heart failure but also provide essential information that will facilitate the development of new epigenetic-based therapies. Nitric oxide epigenetic effects in endothelial cells. In the upper panels it is shown the effect of the nitric oxide donor DETA/NO on the subcellular localization of Histone Deacetylase 4 (HDAC4). HDAC4 shuttles from the cytoplasm to the nucleus of endothelial cells upon DETA/NO treatment. This event corresponds to a marked deacetylation of histone H3 (lower panel; NTG = nitroglycerin). DETA/NO Solvent Specific fields of interest a)Characterization of epigenetic changes associated to aging and to the cellular senescence processes which affect stem cells function; b)Understanding the biological relevance of epigenetic processes involved in heart failure and hypertrophy; c)Investigation of the epigenetic mechanisms underlying the mechanisms of vasorelaxation and nitrate tolerance; d)Identification of genetic and/or pharmacological strategies to modulate chromatin changes associated to diabetes and metabolic memory. 60’ 120’ 240’ 8h HDAC4 DAPI Merge 10% FBS H3AcK14 ctr H3Ph-S10Ac-K14 TSA ctr TSA 30 KD H1 14 KD H3AcK14 NTG - - - - + DAPI Histone modifications are differentially regulated in hypertrophic hearts. Picture shows the effect of Trichostatin A (TSA) administration on acetylation and phospho-acetylation of histone H3 in the hypertrophic heart left ventricle. TSA was cronically administered by subcutaneous minipumps in which an aortic banding was performed to induce cardiac hypertrophy. After 21 days mice were sacrificed and immunofluorescence was performed to detect modified histones. Control hearts did not show any phospho-acetylated histone H3, which were reactivated upon TSA treatment. No differences were observed in the pool of monoacetylated histones H3 betweeen control and treated hearts. 220 CCM — Scientific Report 2011 — Ongoing research 2012 CCM — Scientific Report 2011 — Ongoing research 2012 221 microRNAs in cardiovascular diseases microRNAs (miRNAs) are 21-23-nucleotide non-proteincoding RNA molecules that act as negative regulators of gene expression, modulating the stability and/or the translational efficiency of target messenger RNAs. To date, more than 900 human miRNAs have been cloned and, since each miRNA can modulate hundreds of targets, it may prove difficult to find a biological process or function that is not at least in certain aspects, under the influence of miRNAs. Indeed, miRNA activity is involved in the control of a wide range of biological functions and processes, such as development, differentiation, metabolism, growth, proliferation and apoptosis. miRNAs and oxidative stress. Different tissues and physiological conditions are each associated to a particular pattern of miRNA expression (miRNA signatures) and altered miRNA signatures have been associated to specific diseases. Indeed, our laboratory contributed to the identification of a miRNA signature specific for endothelial cells exposed to reactive oxygen species (ROS). Specifically, we found that the entire miR-200 family expression level increased upon oxidative stress in human umbilical vein endothelial cells (HUVEC) exposed to 200 μM hydrogen peroxide (H2O2) for 8 to 24 hours. Specifically, miRNAs profiling showed that miR-200c and the co-transcribed miR-141 increased more than eightfold. The other clustered miR-200 gene family members (miR-200a, miR-200b and miR-429) were also induced, albeit to a lower level. Furthermore, miR-200c up-regulation was not endothelium restricted, and occurred also in other cell lines and upon exposure to an oxidative stress-inducing drug such as 1,3- bis(2 chloroethyl)-1nitrosourea (BCNU). We found that miR-200c overexpression induced HUVEC growth arrest, apoptosis and senescence. Interestingly, all these phenomena were also induced by H2O2 and were partially rescued by miR-200c inhibition. Moreover, miR-200c target ZEB1 , both messenger RNA and protein, were down-modulated by H2O2 and by miR-200c 222 CCM — Scientific Report 2011 — Ongoing research 2012 overexpression. We also found that ZEB1 knockdown recapitulated miR-200c-induced responses, and that the forced expression of a ZEB1 allele non-targeted by miR-200c was able to prevent miR-200c phenotype (see figure). We also elucidated the mechanism of H2O2mediated miR-200c upregulation, demonstrating the involvement of the oncosuppressor proteins p53 and retinoblastoma. Furthermore, we found that miR-200 family is also induced following acute hindlimb ischemia in skeletal muscles and this induction is oxidative stress dependent, since in p66ShcA-null mice, which exhibit less oxidative stress than wt mice, this induction is significantly attenuated. In conclusion, we demonstrated that ROS induce miR-200c and other miR-200 family members and that the ensuing down-modulation of ZEB1 plays a key role in ROS-induced apoptosis and senescence. miRNAs as biomarker of coronary artery disease. Recent evidence suggests that miRNAs are present in the systemic circulation and may constitute excellent disease biomarkers. Recent results from our laboratory have identified a number of miRNAs (miR-1, -133a, -133b and -499-5p) that increase acutely, both in patients and rodents with myocardial infarction, and return to baseline within a few days after coronary occlusion. This result has led to intense investigation about the possibility that, at least in some clinical conditions, miRNAs may be more sensitive and specific indicators of myocardial infarction than commonly used biomarkers, i.e. cardiac troponins. ZEB1 downmodulation is required for miR-200-c-mediated induction of growth arrest apoptosis and senescence. HUVEC were co-infected with lentiviruses encoding miR-200c and ZEB1D for 2 h. Single infection either of miR-200c or ZEB1D was performed together with ZEB1D backbone vector (vec) or miR-scramble viruses, respectively. Control cells were co-infected with miR-scramble and vec viruses. After infection cells were allowed to recover in complete fresh medium for additional 72 h, without puromycin selection and then plated. (a) Representative western blot demonstrating the expression level of ZEB1 in cells co-infected with miR-200c and ZEB1D miR- 200c forced expression decreased ZEB1, but this effect was largely inhibited in cells expressing ZEB1D. This experiment was performed three times with similar results. Tub, α-tubulin. (b) HUVEC co-infected with miR-200c and ZEB1D showed a higher proliferation rate compared with miR-200c overexpressing cells (n=5 at each time point; *P<0.001; #P<0.05). (c) HUVEC were infected with ZEB1D, miR-200c, miR-200c and ZEB1D, or control viruses. After 72 h, cells were plated and after additional 40 h apoptosis was measured by fragmentation of cellular DNA. The proapoptotic effect of miR-200c was abolished by the expression of ZEB1D (n=3; *P<0.05). (d) HUVEC were infected with ZEB1D, miR-200c, miR-200c and ZEB1D, or control viruses. After 72 h, cells were seeded and after 8 h were fixed and stained for SA-b-gal. Cells co-infected with miR-200c and ZEB1D showed a decrease of the % of SA-βgal-positive cells compared with miR-200c- infected cells (n=3; *P<0.001) CCM — Scientific Report 2011 — Ongoing research 2012 223 Regenerative medicine in cardiovascular diseases Introduction Cardiovascular regenerative medicine represents a major emerging area of investigation. Several key findings have given momentum to cell therapy studies and contributed to the broad interest in this field: • It has been demonstrated that the heart is not a terminally differentiated organ and that, even as part of the physiologic aging process, new cardiac cells form and replace old ones. • It has been identified a c-kit+ resident cardiac stem cell that can differentiate both toward the myocardial and vascular lineages and that, in experimental animal models, can repair the damaged heart following myocardial infarction (MI). • In animal models it has been shown that, beside the c-kit+ cardiac stem cell, other cell types, both cardiac- and bone marrow-derived, once injected into the infarcted heart appear to differentiate toward the myocardial and vascular lineages and improve cardiac function. • Ongoing clinical studies are providing evidence that patients with ischemic heart disease and depressed left ventricular function benefit from autologous bone marrow-derived cell transplantation, their symptoms improve and the function of their heart is better than in control patients. • There is accumulating evidence that in patients with refractory ischemia cardiac injection of bone marrow-derived cells improves symptoms and objective evidence of myocardial perfusion. • Two recent studies have suggested that autologous cardiac cells, c-kit+ and cardiosphere-derived, injected intracoronary in patients with ischemic cardiomyopathy, may have a beneficial action. Historical note. The field of regenerative medicine started in the early 1980s when angiogenic growth factors were discovered and growth factor proteins were used in preclinical studies to induce new blood vessel 224 CCM — Scientific Report 2011 — Ongoing research 2012 formation and enhance blood flow to the ischemic heart and limb. However, these proteins have a short half-life in vivo and the economic cost associated with their prolonged use is exceedingly high. Further, systemic growth factor administration for extended periods of time carries the risk of new blood vessel development in areas where they could be detrimental, such as the retina, brain or subclinical neoplastic foci. These limitations prevented the widespread use of “therapeutic angiogenesis” interventions with proteins. In the early 1990s, gene therapy became an area of intense investigation in regenerative medicine; it appeared to provide a completely novel approach to transfer a gene into the cells of a living organism and to locally enhance the production of a potentially therapeutic protein. This would have avoided the costs of prolonged protein administration and the risks of systemic distribution of the protein. Unfortunately, in clinical experimentation, gene therapy of cardiovascular ischemic diseases met significant failures and only some limited success. This has led to progressive waning in the interest in this potential therapeutic strategy, at least in the cardiovascular arena. Cell therapy entered the regenerative medicine field in the mid-1990s, however it was in 2001 that a pivotal study demonstrated that bone marrow-derived c-kit+/Lin- cells could regenerate the infarcted left ventricle in the mouse. In 2003 another key study demonstrated the existence of a resident c-kit+ cardiac stem cell capable of forming both myocardial cells and blood vessels. Despite the enormous amount of experimental data that both proponents and detractors of cell therapy for cardiovascular diseases have produced, the field has become one of the most intensively debated and investigated, with studies going from clinical experimentation to basic molecular mechanisms of cell transdifferentiation and reprogramming. The road ahead of us. There are a number of challenges that still need to be overcome in order to establish the role of cell therapy in cardiovascular diseases. Which cell is the best one. Cells from different sources are being used in cardiovascular cell therapy studies. At Centro Cardiologico Monzino we use autologous bone marrow-derived CD133+ cells, which have been selected under GMP conditions, to treat patients with refractory myocardial ischemia. Patient enrolment is also open for the use of the same cell type in the treatment of patients with hibernating myocardium undergoing coronary artery bypass surgery. In basic and preclinical studies we have identified and characterized a cardiac mesenchyma-like stromal cell which appears highly prone to differentiate toward the myocardial and vascular lineages and may have a significant therapeutic potential. The Centro Cardiologico Monzino is also investigating the properties of resident cardiac c-kit+ stem cells, for their clinical use, and also induced pluripotent stem cells (iPS) derived from cardiac stromal cells. Ex vivo enhancement of a cell therapeutic potential. Cell transplantation offers the opportunity to manipulate cells ex vivo, prior to reinjecting them into the patient. At Centro Cardiologico Monzino we have focused on the use of epigenetic drugs which modulate chromatin remodelling and gene expression, miRNA manipulation and classical preconditioning interventions to enhance cell plasticity, survival and, ultimately, their therapeutic potential. How cells should be injected. Cell transplant is usually performed either by intracoronary or by direct intramyocardial injection. At Centro Cardiologico Monzino we have elected to use direct intramyocardial injection via the epicardial route. An alternative approach is to inject via the endocardial route in ischemic areas which exhibit electromechanical dissociation and that are identified by NOGA electromechanical mapping. Systemic cell injection and injection into the coronary sinus are also under evaluation by other laboratories. Bone marrow cells mobilization with G-CSF. Recent clinical evidences suggest that mobilization of stem cells from the bone-marrow by granulocyte colonystimulating factor (G-CSF) may improve left ventricular function and remodelling in patients after ST-elevated acute myocardial infarction (STEMI). The mobilization process is not completely understood but the strategy takes advantage to the non-invasive approach of the treatment that seems to mimic the exposure of injured myocardium to higher concentrations of circulating stem and progenitor cells during the first phase after necrosis. The next step will be to corroborate these data with larger and longer-term randomized controlled trials. Drug therapy. The alternative to cell transplantation is represented by drugs that activate the patient’s own stem cells and therefore avoid the need for cell transplant. Few pharmacological interventions have been shown to promote cardiac stem cell activation and cardiac regeneration, i.e the combination of hepatocyte growth factor and insulin-like growth factor 1, thymosin β4 and HMGB1. Centro Cardiologico Monzino has focused on HMGB1; in animal models this protein modulates progenitor cell function, induces cardiac regeneration and improves left ventricular function after acutely MI and also in the chronically failing heart. The other target for pharmacologic intervention is represented by the mechanisms which induce cell cycle arrest; it has been proposed to interfere with these mechanisms to induce adult myocardial cell proliferation. Which diseases should be treated. To date, most studies worldwide have focused on left ventricular dysfunction following MI, i.e. the most common form of heart disease. At Centro Cardiologico Monzino we have treated patients with refractory ischemia and CCM — Scientific Report 2011 — Ongoing research 2012 225 we have consistently found an improvement in angina class and objective evidence of enhanced perfusion (see Figure below). In our preclinical studies we have worked on animal models of acute MI and heart failure secondary to MI. Other laboratories worldwide are working on the use of cell therapy to treat non-ischemic cardiomyopathy, cardiac arrhythmias and pulmonary hypertension. The economic hurdle. The development of any therapeutic intervention requires enormous financial investments and, in the case of drugs and medical devices, the industry supports the research activities, from basic studies to clinical trials. In regenerative medicine the only interest for the industry is in drug therapy and in the development of cell products for allogenic use, as it is presently being done for bone marrow-derived mesenchymal cells. Autologous cell therapy falls in a different category; the financial support comes from taxpayers money and directly from institutions which aim at developing a “service” to offer their patients, somewhat similar to bone marrow transplant. Therefore, finding the financial resources to support autologous cell therapy studies is a major obstacle that has to be overcome in order to bring cell therapy to clinical practice. Publications, Clinical Research Projects, Seminars, Conferences and Courses Conclusions. The studies performed so far have shown the great potential of cardiovascular regenerative medicine. However, many issues have still to be addressed in order to establish regenerative medicine full potential. The ongoing worldwide effort in this field may ultimately lead to cell therapy interventions which best suit each patient’s need. Improvement of myocardial perfusion at stress (see arrows) 6-months after intramyocardial injection of bone-marrow-derived CD133+ cells in a patient with refractory untreatable angina. 226 CCM — Scientific Report 2011 — Ongoing research 2012 CCM — Scientific Report 2011 — Ongoing research 2012 227 Full Papers 2011 AUTHORS TITLE JOURNAL VOLUME PAGE I.F. Avitabile D, Crespi A, Brioschi C, Parente V, Toietta G, Devanna P, Baruscotti M, Truffa S, Scavone A, Rusconi F, Biondi A, D'Alessandra Y, Vigna E, Difrancesco D, Pesce M, Barbuti A. Human cord blood CD34+ progenitor cells acquire functional cardiac properties through a cell fusion process. Am J Physiol Heart Circ Physiol. 300 H18751884 3,88 Banfi C, Brioschi M, Lento S, Pirillo A, Galli S, Cosentino S, Tremoli E, Mussoni L. Statins prevent tissue factor induction by protease-activated receptors 1 and 2 in human umbilical vein endothelial cells in vitro. J Thromb Haemost 9 1608-1619 5,439 Barbieri SS, Amadio P, Gianellini S, Zacchi E, Weksler BB, Tremoli E Tobacco smoke regulates the expression and activity of microsomal prostaglandin E synthase-1: role of prostacyclin and NADPH-oxidase. FASB J 25 3731-3740 6,515 Barbieri SS, Zacchi E, Amadio P, Gianellini S, Mussoni L, Weksler BB, Tremoli E. Cytokines Present in Smokers' Serum Interact with Smoke Components to Enhance Endothelial Dysfunction Cardiovasc Res 90 475-483 6,051 Burba I, Colombo GI, Staszewsky LI, De Simone M, Devanna P, Nanni S, Avitabile D, Molla F, Cosentino S, Russo I, De Angelis N, Soldo A, Biondi A, Gambini E, Gaetano C, Farsetti A, Pompilio G, Latini R, Capogrossi MC, Pesce M. Histone Deacetylase Inhibition Enhances Self Renewal and Cardioprotection by Human Cord Blood-Derived CD34 Cells PLoS One 6 e22158 4,411 Calabresi L, Baldassarre D, Simonelli S, Gomaraschi M, Amato M, Castelnuovo S, Frigerio B, Ravasi A, Sansaro D, Kauhanen J, Rauramaa R, de Faire U, Hamsten A, Smit AJ, Mannarino E, Humphries SE, Giral P, Veglia F, Sirtori CR, Franceschini G, Tremoli E. Plasma lecithin:cholesterol acyltransferase (LCAT) and carotid intima-media thickness in European individuals at high cardiovascular risk J Lipid Res 52 1569-1574 6,115 Cappuzzello C, Di Vito L, Melchionna R, Melillo G, Silvestri L, Cesareo E, Crea F, Liuzzo G, Facchiano A, Capogrossi MC, Napolitano M. Increase of plasma IL-9 and decrease of plasma IL-5, IL-7, and IFN-γ in patients with chronic heart failure. J Transl Med 28 28 3,508 Colombo G, Gertow K, Marenzi G, Brambilla M, De Metrio M, Tremoli E, Camera M. Gene expression profiling reveals multiple differences in platelets from patients with stable angina or non-ST elevation acute coronary syndrome. Thromb Res 128 161-168 2,372 Colussi C, Rosati J, Straino S, Spallotta F, Berni R, Stilli D, Rossi S, Musso E, Macchi E, Mai A, Sbardella G, Castellano S, Chimenti C, Frustaci A, Nebbioso A, Altucci L, Capogrossi MC, Gaetano C. N{varepsilon}-lysine acetylation determines dissociation from GAP junctions and lateralization of connexin 43 in normal and dystrophic heart. Proc Natl Acad Sci USA 108 27952800 9,771 D'Alessandra Y, Pompilio G, Capogrossi M Letter by D'Alessandra et al. regarding article "Circulating microRNA 208b and microRNA 499 reflect myocardial damage in cardiovascular disease" Circ-Cardiovasc Genet 4 e7 4,043 RESEARCH LABORATORIES 228 CCM — Scientific Report 2011 — Ongoing research 2012 CCM — Scientific Report 2011 — Ongoing research 2012 229 230 Di Minno MN, Pezzullo S, Palmieri V, Coppola A, D'Angelo A, Sampietro F, Cavalca V, Tremoli E, Di Minno G. Genotype-independent in vivo oxidative stress following a methionine loading test: Maximal platelet activation in subjects with early-onset thrombosis Thromb Res 128 e43-e48 2,372 Magenta A, Cencioni C, Fasanaro P, Zaccagnini G, Greco S, Sarra-Ferraris G, Antonini A, Martelli F, Capogrossi MC miR-200c is upregulated by oxidative stress and induces endothelial cell apoptosis and senescence via ZEB1 inhibition. Cell Death Differ 18 1628-1639 9,05 Di Minno MN, Russolillo A, Camera M, Brambilla M, De Gregorio A, Tremoli E, Di Minno G New Anti-Thrombotic Drugs for Stroke Prevention. Curr Vasc Pharmacol. 9 723-732 3,184 Marchesi M, Parolini C, Caligari S, Gilio D, Manzini S, Busnelli M, Cinquanta P, Camera M, Brambilla M, Sirtori CR, Chiesa G Br J Pharmacol 164 1460-1468 4,925 Di Rocco G, Gentile A, Antonini A, Ceradini F, Wu JC, Capogrossi MC, Toietta G Enhanced healing of diabetic wounds by topical administration of adipose tissuederived stromal cells overexpressing stromal-derived factor-1: biodistribution and engraftment analysis by bioluminescent imaging. Stem Cells Int 2011 article ID 304562 0 ROSUVASTATIN DOES NOT AFFECT HUMAN APOLIPOPROTEIN A-I EXPRESSION IN GENETICALLY MODIFIED MICE: A CLUE TO THE DISPUTED EFFECT OF STATINS ON HDL. Milano G, Bianciardi P, Rochemont V, Vassalli G, von Segesser LK, Corno AF, Guazzi M, Samaja M Phosphodiesterase-5 inhibition mimics intermittent reoxygenation and improves cardioprotection in the hypoxic myocardium PLoS One 6 e27910 4,411 Franzosi M, Guerrini U, Castiglioni L, Sironi L, Nobili E, Tremoli E, Caiani EG Feasibility of quantitative analysis of regional left ventricular function in the post-infarct mouse by magnetic resonance imaging with retrospective gating. Comput Biol Med 41 829-837 1,112 Minno MN, Guida A, Camera M, Colli S, Minno GD, Tremoli E. Overcoming limitations of current antiplatelet drugs: A concerted effort for more profitable strategies of intervention. Ann Med 43 531-544 4,323 523-529 4,706 Curr Pharm Des 17 3252-3257 4,774 Do statins improve outcomes and delay the progression of non-rheumatic calcific aortic stenosis? 97 Resident cardiac stem cells Parolari A, Tremoli E, Cavallotti L, Trezzi M, Kassem S, Loardi C, Veglia F, Ferrari G, Pacini D, Alamanni F Heart Frati C, Savi M, Graiani G, Lagrasta C, Cavalli S, Prezioso L, Rossetti P, Mangiaracina C, Ferraro F, Madeddu D, Musso E, Stilli D, Rossini A, Falco A, Angelis AD, Rossi F, Urbanek K, Leri A, Kajstura J, Anversa P, Quaini E, Quaini F. Pesce M, Burba I, Gambini E, Prandi F, Pompilio G, Capogrossi MC Endothelial and cardiac progenitors: Boosting, conditioning and (re) programming for cardiovascular repair Pharmacol Ther 129 50-61 8,897 Gambini E, Pompilio G, Biondi A, Alamanni F, Capogrossi MC, Agrifoglio M, Pesce M. C-KIT+ CARDIAC PROGENITORS EXHIBIT MESENCHYMAL MARKERS AND PREFERENTIAL CARDIOVASCULAR COMMITMENT Cardiovasc Res. 89 362-373 5,801 Pozzoli O, Vella P, Iaffaldano G, Parente V, Devanna P, Lacovich M, Lamia CL, Fascio U, Longoni D, Cotelli F, Capogrossi MC, Pesce M. Endothelial Fate and Angiogenic Properties of Human CD34+ Progenitor Cells in Zebrafish Arterioscler Thromb Vasc Biol 31 1589-1597 7,215 Gelosa P, Sevin G, Pignieri A, Budelli S, Castiglioni L, Blanc-Guillemaud V, Lerond L, Tremoli E, Sironi L. Terutroban, a thromboxane/prostaglandin endoperoxide receptor antagonist, prevents hypertensive vascular hypertrophy and fibrosis. Am J Physiol Heart Circ Physiol 300 H762-768 3,88 Rosati J, Spallotta F, Nanni S, Grasselli A, Antonini A, Vincenti S, Presutti C, Colussi C, D'Angelo C, Biroccio A, Farsetti A, Capogrossi MC, Illi B, Gaetano C Smad-Interacting Protein-1 and MicroRNA 200 Family Define a Nitric OxideDependent Molecular Circuitry Involved in Embryonic Stem Cell Mesendoderm Differentiation. Arterioscler Thromb Vasc Biol 31 898-907 7,215 Gentile A, Toietta G, Pazzano V, Tsiopoulos VD, Giglio AF, Crea F, Pompilio G, Capogrossi MC, Di Rocco G. Human epicardium-derived cells fuse with high efficiency with skeletal myotubes and differentiate towards the skeletal muscle phenotype: A comparison study with stromal and endothelial cells. Mol Biol Cell 22 581-592 5,861 Rossini A, Frati C, Lagrasta C, Graiani G, Scopece A, Cavalli S, Musso E, Baccarin M, Di Segni M, Fagnoni F, Germani A, Quaini E, Mayr M, Xu Q, Barbuti A, Difrancesco D, Pompilio G, Quaini F, Gaetano C, Capogrossi MC. Human Cardiac And Bone Marrow Stromal Cells Exhibit Distinctive Properties Related To Their Origin. Cardiovasc Res. 89 650-660 5,801 Gertow K, Nobili E, Folkersen L, Newman JW, Pedersen TL, Ekstrand J, Swedenborg J, Kühn H, Wheelock CE, Hansson GK, Hedin U, Haeggström JZ, Gabrielsen A 12- and 15-lipoxygenases in human carotid atherosclerotic lesions: Associations with cerebrovascular symptoms Atherosclerosis 215 411-416 4,086 Squellerio I, Tremoli E, Cavalca V Quantification of arginine and its metabolites in human erythrocytes using liquid chromatography-tandem mass spectrometry Anal Biochem 412 108-110 3,236 Gianella A, Jarzyna PA, Mani V, Ramachandran S, Calcagno C, Tang J, Kann B, Dijk WJ, Thijssen VL, Griffioen AW, Storm G, Fayad ZA, Mulder WJ Multifunctional nanoemulsion platform for imaging guided therapy evaluated in experimental cancer ACS Nano 5 44224433 9,855 Agostoni P, Apostolo A, Sciomer S Respir Physiol Neurobiol 179 127-128 2,382 Giuliani A, Frati C, Rossini A, Komlev VS, Lagrasta C, Savi M, Cavalli S, Gaetano C, Quaini F, Manescu A, Rustichelli F. High-resolution X-ray microtomography for three-dimensional imaging of cardiac progenitor cell homing in infarcted rat hearts J Tissue Eng Regen Med. Evolution of the concept of ventilatory limitation during exercise. Combining the pneumologist and cardiologist point of view 37 841-847 5,527 NO points to epigenetics in vascular development. Cardiovasc Res 90 447-456 6,051 Surfactant protein SPB and RAGE increases in the plasma during cardiopulmonary by-pass: a pilot study Eur Respir J. Illi B, Colussi C, Rosati J, Spallotta F, Nanni S, Farsetti A, Capogrossi MC, Gaetano C Agostoni P, Banfi C, Brioschi M, Magrì D, Sciomer S, Berna G, Brambillasca C, Marenzi G, Sisillo E. 256-260 2,382 Prog Cardiovasc Dis 53 334-343 4,841 Kinetics of plasma SPB and RAGE during mechanical ventilation in patients undergoing major vascular surgery 178 Investigating air pollution and atherosclerosis in humans: concepts and outlook Agostoni P, Banfi C, Magrì D, Vignati C, Doria E, Salvioni E, Moliterni P, Marenzi G, Tremoli E, Sisillo E. Respir Physiol Neurobiol Künzli N, Perez L, von Klot S, Baldassarre D, Bauer M, Basagana X, Breton C, Dratva J, Elosua R, de Faire U, Fuks K, de Groot E, Marrugat J, Penell J, Seissler J, Peters A, Hoffmann B Agostoni P, Contini M L'adattamento alla quota nel paziente con insufficienza cardiaca CardioRenal Journal 62-63 0 Limana F, Capogrossi MC, Germani A. The epicardium in cardiac repair: From the stem cell view. Pharmacol Ther 129 82-96 8,897 Agostoni P, Swenson ER, Bussotti M, Revera M, Meriggi P, Faini A, Lombardi C, Bilo G, Giuliano A, Bonacina D, Modesti PA, Mancia G, Parati G High altitude exposure of three weeks duration increases lung diffusing capacity in humans J Appl Physiol 1564-1571 4,232 Limana F, Esposito G, D'Arcangelo D, Di Carlo A, Romani S, Melillo G, Mangoni A, Bertolami C, Pompilio G, Germani A, Capogrossi MC HMGB1 Attenuates Cardiac Remodelling in the Failing Heart via Enhanced Cardiac Regeneration and miR-206-Mediated Inhibition of TIMP-3 PLoS One 6 e19845 4,411 CCM — Scientific Report 2011 — Ongoing research 2012 5 e168-e178 CRITICAL CARDIOLOGY 3,534 110 CCM — Scientific Report 2011 — Ongoing research 2012 231 232 Alexander JH, Lopes RD, James S, Kilaru R, He Y, Mohan P, Bhatt DL, Goodman S, Verheugt FW, Flather M, Huber K, Liaw D, Husted SE, Lopez-Sendon J, De Caterina R, Jansky P, Darius H, Vinereanu D, Cornel JH, Cools F, Atar D, Leiva-Pons JL, Keltai M, Ogawa H, Pais P, Parkhomenko A, Ruzyllo W, Diaz R, White H, Ruda M, Geraldes M, Lawrence J, Harrington RA, Wallentin L; the APPRAISE-2 Investigators Apixaban with Antiplatelet Therapy after Acute Coronary Syndrome N Engl J Med Bellotto F, Compostella L, Agostoni P, Torregrossa G, Setzu T, Gambino A, Russo N, Feltrin G, Tarzia V, Gerosa G. Peripheral adaptation mechanisms in physical training and cardiac rehabilitation: the case of a patient supported by a cardiowest total artificial heart. J Card Fail 17 670-675 Boccanelli A, Agostoni P Lo studio EMPHASIS-HF G Ital cardiol 12 Cattadori G, Salvioni E, Gondoni E, Agostoni P. Evaluation of noninvasive exercise cardiac output determination in chronic heart failure patients: a proposal of a new diagnostic and prognostic method. J Cardiovasc Med (Hagerstown). 12 Cattadori G, Schmid JP, Brugger N, Gondoni E, Palermo P, Agostoni P. Hemodynamic effects of exercise training in heart failure J Card Fail 17 916-922 3,362 Cristell N, Cianflone D, Durante A, Ammirati E, Vanuzzo D, Banfi M, Calori G, Latib A, Crea F, Marenzi G, De Metrio M, Moretti L, Li H, Uren NG, Hu D, Maseri A; FAMI Study Investigators. High-Sensitivity C-Reactive Protein Is Within Normal Levels at the Very Onset of First ST-Segment Elevation Acute Myocardial Infarction in 41% of Cases A Multiethnic Case-Control Study. J Am Coll Cardiol 58 26542661 14,292 Magini A, Apostolo A, Italiano G, Agostoni P Misurazione della diffusione alveolocapillare: da strumento diagnostico a strumento prognostico e terapeutico CardioRenal Journal Magrì D, Palermo P, Cauti FM, Contini M, Farina S, Cattadori G, Apostolo A, Salvioni E, Magini A, Vignati C, Alimento M, Sciomer S, Bussotti M, Agostoni P. Chronotropic Incompentence and Functional Capacity in Chronic Heart Failure: No Role of beta-Blockers and beta-Blocker Dose Cardiovasc Ther. Marenzi G How safe are iodinated contrast media? Daily Congress News Marenzi G, De Metrio M, Bartorelli AL. Author's reply to Acute hyperglycemia: Is really a new risk marker for contrastinduced nephropathy in patients with acute myocardial infarction without diabetes and normal renal function? Am Heart J Metra M, Zacà V, Parati G, Agostoni P, Bonadies M, Ciccone M, Cas AD, Iacoviello M, Lagioia R, Lombardi C, Maio R, Magrì D, Musca G, Padeletti M, Perticone F, Pezzali N, Piepoli M, Sciacqua A, Zanolla L, Nodari S, Filardi PP, Dei Cas L; on behalf of the Heart Failure Study Group of the Italian Society of Cardiology. Cardiovascular and noncardiovascular comorbidities in patients with chronic heart failure J Cardiovasc Med (Hagerstown) Modesti PA, Rapi S, Paniccia R, Bilo G, Revera M, Agostoni P, Piperno A, Cambi GE, Rogolino A, Biggeri A, Mancia G, Gensini GF, Abbate R, Parati G. Index measured at an intermediate altitude to predict impending Acute Mountain Sickness Med Sci Sports Exerc 43 1811-1818 4,106 Patel MR, Mahaffey KW, Garg J, Pan G, Singer DE, Hacke W, Breithardt G, Halperin JL, Hankey GJ, Piccini JP, Becker RC, Nessel CC, Paolini JF, Berkowitz SD, Fox KA, Califf RM; ROCKET AF Investigators Rivaroxaban versus warfarin in nonvalvular atrial fibrillation N Engl J Med 365 883-891 52,362 Sisillo E, Marenzi G N-Acetylcysteine for the Prevention of Acute Kidney Injury After Cardiac Surgery. J Clin Pharmacol 51 Zannad F, McMurray JJ, Krum H, van Veldhuisen DJ, Swedberg K, Shi H, Vincent J, Pocock SJ, Pitt B; EMPHASIS-HF Study Group. Eplerenone in patients with systolic heart failure and mild symptoms. N Engl J Med 364 CCM — Scientific Report 2011 — Ongoing research 2012 365 30 52,362 Biondi-Zoccai G, Sheiban I, Moretti C, Palmerini T, Marzocchi A, Capodanno D, Tamburino C, Margheri M, Vecchi G, Sangiorgi G, Santarelli A, Bartorelli AL, Briguori C, Vignali L, Pede FD, Ramondo A, Medda M, de Carlo M, Falsini G, Benassi A, Palmieri C, Filippone V, Sangiorgi D, Barlocco F, de Servi S. Appraising the impact of left ventricular ejection fraction on outcomes of percutaneous drug-eluting stenting for unprotected left main disease: insights from a multicenter registry of 975 patients Clin Res Cardiol. 100 403-411 2,958 3,362 Cuculi F, Banning AP, Abizaid A, Bartorelli AL, Baux AC, Dzavík V, Ellis S, Gao R, Holmes D, Jeong MH, Legrand V, Neumann FJ, Nyakern M, Spaulding C, Stoll HP, Worthley S, Urban P Outcomes in patients undergoing multivessel percutaneous coronary intervention using sirolimus-eluting stents: a report from the e-SELECT registry EuroIntervention 7 962-968 0 315-318 0 Fabbiocchi F, Pirondini M, Trabattoni D, Ferrari C, Bartorelli A EuroIntervention 19-27 0,712 How should I treat a patient with lifethreatening gastrointestinal bleeding early after coronary drug-eluting stent implantation Garg S, Serruys PW, Silber S, Wykrzykowska J, van Geuns RJ, Richardt G, Buszman PE, Kelbæk H, van Boven AJ, Hofma SH, Linke A, Klauss V, Wijns W, Macaya C, Garot P, Dimario C, Manoharan G, Kornowski R, Ischinger T, Bartorelli A, Van Remortel E, Ronden J, Windecker S. The Prognostic Utility of the SYNTAX Score on 1-Year Outcomes After Revascularization With Zotarolimus- and Everolimus-Eluting Stents A Substudy of the RESOLUTE All Comers Trial. JACC Cardiovascular Interv 4 432-441 5,862 Hong YJ, Jeong MH, Abizaid A, Banning A, Bartorelli A, Dzavik V, Ellis SG, Gao R, Holmes DR Jr, Legrand V, Neumann FJ, Spaulding C, Worthley S, Urban P; e-SELECT Registry Investigators Sirolimus-Eluting Coronary Stents in Octogenarians A 1-Year Analysis of the Worldwide e-SELECT Registry JACC Cardiovascular Interv 4 982-991 5,862 Martinoni A, De Servi S, Boschetti E, Zanini R, Palmerini T, Politi A, Musumeci G, Belli G, De Paolis M, Ettori F, Piccaluga E, Sangiorgi D, Repetto A, D'Urbano M, Castiglioni B, Fabbiocchi F, Onofri M, De Cesare N, Sangiorgi G, Lettieri C, Poletti F, Pirelli S, Klugmann S. Importance and limits of pre-hospital electrocardiogram in patients with ST elevation myocardial infarction undergoing percutaneous coronary angioplasty. Eur J Cardiovasc Prev Rehabil 18 526-532 2,638 Massari FA, Trabattoni D, Gianni C, Tonella T, Khirani S, Magrini F Onda T negativa post extrasistolica: significato ischemico? It J Practice Cardiol 1 2-6 0 Montorsi P, Caputi L, Galli S, Ciceri E, Ballerini G, Agrifoglio M, Ravagnani P, Trabattoni D, Pontone G, Fabbiocchi F, Loaldi A, Parati E, Andreini D, Veglia F, Bartorelli AL. Microembolization during carotid artery stenting in patients with high-risk, lipid-rich plaque a randomized trial of proximal versus distal cerebral protection. J Am Coll Cardiol 58 1656-1663 14,292 Politi A, Martinoni A, Klugmann S, Zanini R, Onofri M, Guagliumi G, Fiorentini C, Lettieri C, Belli G, Piccaluga E, De Cesare N, Dʼurbano M, Ettori F, Repetto A, Musumeci G, Castiglioni B, Colombo P, Passamonti E, Bramucci E, Cattaneo L, Ferrari G, Repetto S, Bartorelli A, Pirelli S, De Servi S; on behalf of the LombardIMA Study Group LombardIMA: a regional registry for coronary angioplasty in ST-elevation myocardial infarction. J Cardiovasc Med (Hagerstown). 12 43-50 0,712 Silber S, Windecker S, Vranckx P, Serruys PW; RESOLUTE All Comers investigators. Collaborators: Windecker S, Serruys PW, Richardt G, Kelbaek H, van Boven AJ, Linke A, Buszman PE, Klauss V, Sohn HY, Silber S, Wijns W, Macaya C, DiMario C, Manoharan G, Kornowski R, Garot P, Ischinger T, Leber AW, Garot P, Bartorelli AL. Unrestricted randomised use of two new generation drug-eluting coronary stents: 2-year patient-related versus stentrelated outcomes from the RESOLUTE All Comers trial Lancet 377 1241-1247 33,633 33-36 0 100-108 2,741 12-13 0 162 12 INTERVENTIONAL CARDIOLOGY 5,052 76-78 0,712 3,59 11-21 0 52,362 CCM — Scientific Report 2011 — Ongoing research 2012 233 Stefanini GG, Serruys PW, Silber S, Khattab AA, van Geuns RJ, Richardt G, Buszman PE, Kelbæk H, van Boven AJ, Hofma SH, Linke A, Klauss V, Wijns W, Macaya C, Garot P, Di Mario C, Manoharan G, Kornowski R, Ischinger T, Bartorelli AL, Gobbens P, Windecker S The Impact of Patient and Lesion Complexity on Clinical and Angiographic Outcomes After Revascularization With Zotarolimus- and Everolimus-Eluting Stents A Substudy of the RESOLUTE All Comers Trial (A Randomized Comparison of a Zotarolimus-Eluting Stent With an Everolimus-Eluting Stent for Percutaneous Coronary Intervention). J Am Coll Cardiol Trabattoni D, Bartorelli A IVUS nella guida all'ìmpianto di DES: quando, come e perché utilizzarlo Trabattoni D, Fabbiocchi F, Galli S, Montorsi P, Lualdi A, Grancini L, Ravagnani P, Bartorelli AL Sex difference in long-term clinical outcome after sirolimus-eluting stent implantation Coron Artery Dis Trabattoni D, Fabbiocchi F, Montorsi P, Galli S, Teruzzi G, Grancini L, Gatto P, Bartorelli AL Sustained long-term benefit of patent foramen ovale closure on migraine Trabattoni D, Gatto P, Bartorelli AL. Trabattoni D, Montorsi P, Fabbiocchi F, Lualdi A, Gatto P, Bartorelli AL 57 2221-2232 14,292 23-29 0 22 442-446 1,665 Catheter Cardiovasc Interv 77 570-574 2,398 A new kaolin-based hemostatic bandage use after coronary diagnostic and interventional procedures. Int J Cardiol 21 1687-1691 3,469 A new kaolin-based haemostatic bandage compared with manual compression for bleeding control after percutaneous coronary procedures. Eur Radiol 21 1687-1691 3,594 Stent Thrombosis and Bleeding Complications After Implantation of Sirolimus-Eluting Coronary Stents in an Unselected Worldwide Population A Report From the e-SELECT (Multi-Center Post-Market Surveillance) Registry J Am Coll Cardiol Landoni G, Augoustides JG, Guarracino F, Santini F, Ponschab M, Pasero D, Rodseth RN, Biondi-Zoccai G, Silvay G, Salvi L, Camporesi E, Comis M, Conte M, Bevilacqua S, Cabrini L, Cariello C, Caramelli F, DE Santis V, Del Sarto P, Dini D, Forti A, Galdieri N, Giordano G, Gottin L, Greco M, Maglioni E, Mantovani L, Manzato A, Meli M, Paternoster G, Pittarello D, Rana KN, Ruggeri L, Salandin V, Sangalli F, Zambon M, Zucchetti M, Bignami E, Alfieri O, Zangrillo A. Mortality reduction in cardiac anesthesia and intensive care: results of the first International Consensus Conference Acta Anaesthesiol Scand Agrifoglio M, Cappai A, Filippi N, Alamanni F Penetrating atherosclerotic ulcer of the ascending aorta: the role of computed tomography scan J Cardiovasc Med Agrifoglio M, Filippini S, Roberto M, Zanobini M, Gregorini L, Alamanni F. Non Infective Severe Aortic Paravalvular Leakage 7 Years After Surgery: The Role of Suture Technique J Cardiothorac Surg 6 60 0,908 Agrifoglio M, Pontone G, Andreini D, Biglioli P, Cheema FH, Barili F Conservative management of the pseudoaneurysms of ascending aortic graft: a case of spontaneous regression at follow-up. J Cardiovasc Med 12 586-588 0,786 Agrifoglio M, Zoli S, Cappai A, Trabattoni P, Spirito R, Biglioli P. Endovascular Treatment of Abdominal Aortic Aneurysm After Previous Left Pneumonectomy: A Sound Choice. Ann Vasc Surg 25 556e7-10 1,332 D'Onofrio A, Fusari M, Abbiate N, Zanchettin C, Bianco R, Fabbri A, Salvador L, Polesel E, Biglioli P, Gerosa G Transapical aortic valve implantation in high-risk patients with severe aortic valve stenosis Ann Thorac Surg 92 1671-1677 3,792 D'Onofrio A, Rubino P, Fusari M, Salvador L, Musumeci F, Rinaldi M, Vitali EO, Glauber M, Di Bartolomeo R, Alfieri OR, Polesel E, Aiello M, Casabona R, Livi U, Grossi C, Cassese M, Pappalardo A, Gherli T, Stefanelli G, Faggian GG, Gerosa G. Clinical and hemodynamic outcomes of "all-comers" undergoing transapical aortic valve implantation: Results from the Italian Registry of Trans-Apical Aortic Valve Implantation (I-TA). J Thoracic Cardiovasc Surg 142 768-775 3,608 Urban P, Abizaid A, Banning A, Bartorelli AL, Baux AC, Džavík V, Ellis S, Gao R, Holmes D, Jeong MH, Legrand V, Neumann FJ, Nyakern M, Spaulding C, Worthley S; e-SELECT Investigators. 57 1445-1454 14,292 CARDIOVASCULAR SURGERY 234 CCM — Scientific Report 2011 — Ongoing research 2012 55 12 259-266 671-672 2,196 Dainese L, Cappai A, Biglioli P Recurrent pericardial effusion after cardiac surgery: the use of colchicine after recalcitrant conventional therapy J Cardiothorac Surg 6 96 0,908 Dogliotti G, Dozio E, Agrifoglio M, Costa E, Broich G, Malavazos AE, Palumbo F, Corsi MM Italian Air Force acrobatic pilots are protected against flight-induced oxidative stress In Vivo 25 1013-1018 1,159 Kassem S, Alamanni F, Moasis GA Eagle-shaped patch to restore mitralaortic continuity J Thorac Cardiovasc Surg 141 1321-1323 3,063 Kassem S, Jamil H Papillary muscle-to-anterior annulus stitches: Another technique to prevent systolic anterior motion after mitral valve repair J Thorac Cardiovasc Surg 142 1278-1281 3,608 Kassem S, Moasis GA, Biglioli P. Tent-shape technique: another procedure to repair P2 of posterior leaflet of mitral valve Eur J Cardiothorac Surg 39 1064-1066 2,397 Kassem S, Othman M Annulus-edge-papillary stitch to repair P2 of the mitral valve posterior leaflet. J Thorac Cardiovasc Surg 141 e45-47 3,608 Kassem S, Othman M, Polvani G Paradoxical artificial cords: new technique to prevent systolic anterior motion post mitral valve reconstructions J Clinic Experiment Cardiol Loardi C, Alamanni F, Trezzi M, Kassem S, Cavallotti L, Tremoli E, Pacini D, Parolari A Biology of mitral valve prolapse: The harvest is big, but the workers are few. Int J Cardiol 151 129-135 3,469 Maggiolini S, Lenatti L, Malafronte C, Pompilio G, Righetti S, Achilli F. G-CSF administration in acute myocardial infarction: what is the best timing? Cardiovasc Res 91 180 6,051 Pompilio G, Filippini S, Agrifoglio M, Merati E, Lauri G, Salis S, Alamanni F, Parolari A Determinants of pericardial drainage for cardiac tamponade following cardiac surgery Eur J Cardio-Thorac Surg 39 e107-e113 2,293 Ripa A, Fusari M, Alamanni F, Biglioli P, Caraceni D, Capparuccia C, Antonicelli R Long term results of percutaneous aortic valve implant in a 90-year-old patient J Cardiovasc Surg 52 754-755 1,352 Scacciatella P, Amato G, Ebrille E, Levis M, Frisenda V, Pompilio G, Marra S Current perspectives in cell therapy in cardiology: an overview of ongoing trials G Ital Cardiol (Rome). 11 769-774 0 Wendler O, Walther T, Schroefel H, Lange R, Treede H, Fusari M, Rubino P, Thomas M The SOURCE Registry: what is the learning curve in trans-apical aortic valve implantation? Eur J Cardiothorac Surg 39 853-859 2,397 Zanobini M L'aneurisma postinfartuale del ventricolo sinistro 50 10-11 0 Zanobini M, Cavallotti L Aneurisma post-infartuale del ventricolo sinistro: l'importanza del team cardiochirurgo-elettrofisiologo HF Informer 23-25 0 Zoli S, Kassem S, Tessitore G, Annoni A, Alamanni F, Agrifoglio M. Mycotic Ascending Aortic Pseudoaneurysm following Reduction Aortoplasty J Card Surg 26 100-101 1,16 Bai R, Di Biase L, Shivkumar K, Mohanty P, Tung R, Santangeli P, Saenz LC, Vacca M, Verma A, Khaykin Y, Mohanty S, Burkhardt JD, Hongo R, Beheiry S, Dello Russo A, Casella M, Pelargonio G, Santarelli P, Sanchez J, Tondo C, Natale A. Ablation of Ventricular Arrhythmias in Arrhythmogenic Right Ventricular Dysplasia/Cardiomyopathy: ArrhythmiaFree Survival after Endo-Epicardial Substrate Based Mapping and Ablation Circ Arrhythm Electrophysiol. 4 478-485 4,78 Bartoletti S, Pelargonio G, Dello Russo A, Casella M, Tondo C. To the Editor: PACE -Pacing Clin Electrophysiol 34 1707 1,353 Bertaglia E, Berto P, Bongiorni MG, Catanzariti D, De Fabrizio G, De Ponti R, Grimaldi M, Pandozi C, Tondo C, Gulizia M. Catheter ablation of atrial fibrillation: Health Technology Assessment Report from the Italian Association of Arrhythmology and Cardiac Pacing (AIAC) G Ital Cardiol (Rome) 12 726-776 0 0,786 0 ELECTROPHYSIOLOGY CCM — Scientific Report 2011 — Ongoing research 2012 235 Botto GL, Boriani G, Favale S, Landolina M, Molon G, Tondo C, Biffi M, Grandinetti G, De Filippo P, Raciti G, Padeletti L. Treatment of atrial fibrillation with a dual defibrillator in heart failure patients (TRADE HF): protocol for a randomized clinical trial Trials 12 44 2,08 Casella M, Bartoletti S, Dello Russo A, Tondo C 9 pregnant women with drug-refractory supraventricular tachyarrhythmias. Catheter ablation during pregnancy J Cardiovasc Electrophysiol 21 E80 Casella M, Carbucicchio C, Dello Russo A, Tundo F, Bartoletti S, Monti L, Marana I, Giraldi F, Tondo C. Radiofrequency catheter ablation of life-threatening ventricular arrhythmias caused by left ventricular metastatic infiltration Circ Arrhythm Electrophysiol 4 e7-e10 Casella M, Pelargonio G, Dello Russo A, Riva S, Bartoletti S, Santangeli P, Scarà A, Sanna T, Proietti R, Di Biase L, Gallinghouse GJ, Narducci ML, Sisto L, Bellocci F, Natale A, Tondo C. Near-zero fluoroscopic exposure in supraventricular arrhythmia ablation using the EnSite NavX mapping system: personal experience and review of the literature J Interv Card Electrophysiol 31 Dello Russo A, Casella M, Carbucicchio C, Tondo C Scar mapping for risk stratification of sudden cardiac death: where are we now? Card Electrophysiol Clin 3 539-547 0 Dello Russo A, Pieroni M, Santangeli P, Bartoletti S, Casella M, Pelargonio G, Smaldone C, Bianco M, Di Biase L, Bellocci F, Zeppilli P, Fiorentini C, Natale A, Tondo C. Concealed Cardiomyopathies In Competitive Athletes With Ventricular Arrhythmias And An Apparently Normal Heart: Role Of Cardiac Electroanatomic Mapping And Biopsy. Heart Rhythm 8 1915-1922 4,246 Di Biase L, Al-Ahamad A, Santangeli P, Hsia HH, Sanchez J, Bai R, Bailey S, Horton R, Gallinghouse GJ, Burkhardt DJ, Lakkireddy D, Yang Y, Badhwar N, Scheinman M, Tung R, Dello Russo A, Pelargonio G, Casella M, Tomassoni G, Shivkumar K, Natale A. Safety and outcomes of cryoablation for ventricular tachyarrhythmias: results from a multicenter experience Heart Rhythm 8 968-974 4,246 Forleo GB, Pappalardo A, Avella A, Visigalli L, Dello Russo A, Tondo C. Real-time integration of intracardiac echocardiography and 3D electroanatomical mapping to guide catheter ablation of isthmus-dependent atrial flutter in a patient with complete situs inversus and interruption of the inferior vena cava with azygos continuation. J Interv Card Electrophysiol Long-term effectiveness of cardiac resynchronization therapy in heart failure patients with unfavorable cardiac veins anatomy comparison of surgical versus hemodynamic procedure. J Am Coll Cardiol Narducci ML, Pelargonio G, Dello Russo A, Casella M, Biasucci LM, La Torre G, Pazzano V, Santangeli P, Baldi A, Liuzzo G, Tondo C, Natale A, Crea F Role of tissue C-reactive protein in atrial cardiomyocytes of patients undergoing catheter ablation of atrial fibrillation: pathogenetic implications Europace 13 Santangeli P, Dello Russo A, Casella M, Pelargonio G, Di Biase L, Natale A Left ventricular ejection fraction for the risk stratification of sudden cardiac death: friend or foe? Intern Med J Santangeli P, Di Biase L, Pelargonio G, Dello Russo A, Casella M, Bartoletti S, Burkhardt JD, Mohanty P, Santarelli P, Natale A Cardiac resynchronization therapy in patients with mild heart failure: a systematic review and meta-analysis Santangeli P, Di Biase L, Pelargonio G, Dello Russo A, Casella M, Sanchez J, Horton R, Gallinghouse GJ, Natale A Santangeli P, Hamilton-Craig C, Dello Russo A, Pieroni M, Casella M, Pelargonio G, Biase LD, Smaldone C, Bartoletti S, Narducci ML, Tondo C, Bellocci F, Natale A Giraldi F, Cattadori G, Roberto M, Carbucicchio C, Pepi M, Ballerini G, Alamanni F, Della Bella P, Pontone G, Andreini D, Tondo C, Agostoni PG 236 Smaldone C, Pieroni M, Pelargonio G, Dello Russo A, Palmieri V, Bianco M, Gentile M, Crea F, Bellocci F, Zeppilli P Left-dominant arrhythmogenic cardiomyopathy Circ Arrhythm Electrophysiol 4 e29-32 4,78 Tung R, Nakahara S, Maccabelli G, Buch E, Wiener I, Boyle NG, Carbucicchio C, Bella PD, Shivkumar K. Ultra High-Density Multipolar Mapping With Double Ventricular Access: A Novel Technique for Ablation of Ventricular Tachycardia J Cardiovasc Electrophysiol. 22 49-56 3,703 3,288 4,78 CARDIOVASCULAR IMAGING Andreini D, Mushtaq S, Pontone G, Cortinovis S, Annoni A, Formenti A, Agostoni P, Bartorelli AL, Fiorentini C, Ballerini G, Pepi M Additional clinical role of 64-slice multidetector computed tomography in the evaluation of coronary artery variants and anomalies. Int J Cardiol 12 388-390 3,469 Andreini D, Pontone G, Bartorelli AL, Mushtaq S, Trabattoni D, Bertella E, Cortinovis S, Annoni A, Formenti A, Ballerini G, Agostoni P, Fiorentini C, Pepi M. High diagnostic accuracy of prospective ECG-gating 64-slice computed tomography coronary angiography for the detection of in-stent restenosis : In-stent restenosis assessment by lowdose MDCT. Eur Radiol 21 1430-1438 3,594 Andreini D, Pontone G, Formenti A, Agnifili M, Mushtaq S, Pepi M Complementary role of cardiac computed tomography and Dopplerechocardiography in the evaluation of an uncommon case of giant pseudoaneurysm of ascending aorta complicated by fistula to the pulmonary artery J Cardiovasc Med 12 173-175 0,712 Ben Zekry S, Saad RM, Ozkan M, Al Shahid MS, Pepi M, Muratori M, Xu J, Little SH, Zoghbi WA. Flow acceleration time and ratio of acceleration time to ejection time for prosthetic aortic valve function. JACC Cardiovasc Imaging 4 1161-1170 5,528 Caiani EG, Fusini L, Veronesi F, Tamborini G, Maffessanti F, Gripari P, Corsi C, Naliato M, Zanobini M, Alamanni F, Pepi M Quantification of mitral annulus dynamic morphology in patients with mitral valve prolapse undergoing repair and annuloplasty during a 6 month follow-up Eur J Echocardiogr 12 375-383 2,117 Ewe SH, Muratori M, Delgado V, Pepi M, Tamborini G, Fusini L, Klautz RJ, Gripari P, Bax JJ, Fusari M, Schalij MJ, Ajmone Marsan N Hemodynamic and Clinical Impact of Prosthesis-Patient Mismatch After Transcatheter Aortic Valve Implantation. J Am Coll Cardiol 58 Feasibility of Intraoperative ThreeDimensional Transesophageal Echocardiography in the Evaluation of Right Ventricular Volumes and Function in Patients Undergoing Cardiac Surgery. J Am Soc Echocardiogr 24 868-877 3,518 14,292 Fusini L, Tamborini G, Gripari P, Maffessanti F, Mazzanti V, Muratori M, Salvi L, Sisillo E, Caiani EG, Alamanni F, Fiorentini C, Pepi M 24 405-413 3,518 1,839 Quantitative Analysis of Mitral Valve Apparatus in Mitral Valve Prolapse Before and after Annuloplasty: A Three-Dimensional Intraoperative Transesophageal Study. J Am Soc Echocardiogr 1133-1140 Maffessanti F, Marsan NA, Tamborini G, Sugeng L, Caiani EG, Gripari P, Alamanni F, Jeevanandam V, Lang RM, Pepi M. 251-254 6,802 1,626 J Interv Card Electrophysiol 32 125-135 1,228 Multidetector computed tomography vs multiplane transesophageal echocardiography in detecting atrial Thrombi in patients candidate to radiofrequency ablation of atrial fibrillation 152 55-60 Maltagliati A, Pontone G, Annoni A, Formenti A, Galli CA, Tamborini G, Alimento M, Andreini D, Tondo C, Pepi M Int J Cardiol 41 161 314-321 5,052 J Interv Card Electrophysiol 31 69-80 1,228 Left atrial reverse remodeling and functional improvement after mitral valve repair in degenerative mitral regurgitation: A real-time 3-dimensional echocardiography study Am Heart J Catheter ablation of atrial fibrillation: randomized controlled trials and registries, a look back and the view forward Marsan NA, Maffessanti F, Tamborini G, Gripari P, Caiani E, Fusini L, Muratori M, Zanobini M, Alamanni F, Pepi M. Pepi M, Tamborini G, Fusini L, Maffessanti F 21 109-117 0 J Cardiovasc Electrophysiol 22 1359-1366 3,288 Three-dimensional echocardiography and mitral valve prolapse diagnosis: new insights into leaflet and cardiac chamber morphology, and annulus dynamics J Cardiovsc Echogr Imaging of Scar in Patients with Ventricular Arrhythmias of Right Ventricular Origin: Cardiac Magnetic Resonance Versus Electroanatomic Mapping CCM — Scientific Report 2011 — Ongoing research 2012 30 58 109-118 273-277 483-490 1,228 1,228 14,292 CCM — Scientific Report 2011 — Ongoing research 2012 237 Pontone G, Andreini D, Bartorelli AL, Annoni A, Mushtaq S, Bertella E, Formenti A, Cortinovis S, Alamanni F, Fusari M, Bona V, Tamborini G, Muratori M, Ballerini G, Fiorentini C, Biglioli P, Pepi M Feasibility and accuracy of a comprehensive multidetector computed tomography acquisition for patients referred for balloon-expandable transcatheter aortic valve implantation Am Heart J 161 1106-1113 5,052 Pontone G, Andreini D, Bartorelli AL, Bertella E, Mushtaq S, Cortinovis S, Chiappa L, Annoni A, Formenti A, Trabattoni D, Montorsi P, Ballerini G, Fiorentini C, Pepi M. Comparison between low-dose multidetector computed coronary angiography and myocardial perfusion imaging test in patients with intermediate pre-test likelihood of coronary artery disease Int J Cardiol 147 454-457 6,802 Pontone G, Andreini D, Bertella E, Cortinovis S, De Martini S, Pirondini M, Fabbiocchi F, Bartorelli AL, Pepi M. Detection of left main coronary artery anomalous origin with low-dose multidetector computed tomography using prospective ECG gating. J Cardiovasc Med 12 506-509 0,786 Pontone G, Andreini D, Galli S, Montorsi P, Bartorelli AL, Pepi M Detection of a large left anterior descending coronary artery aneurysm using low-dose coronary multidetector computed tomography. J Cardiovasc Med Detection of bronchocoronary collateral by low-dose multidetector computed tomography. Eur J Cardiothor Surg Pontone G, Grancini L, Andreini D, Pepi M. Clinical Research Projects in Progress during 2011 0,712 Title Principal Investigator RESEARCH LABORATORIES 40 272 2,397 Erythrocyte NO metabolic pathway in patients with microvascular angina Cavalca Effect of acute hyperglycemia on the synthesis pathway of nitrogen monoxide (NO) in erythrocytes Cavalca Effect of aspirin chronic treatment on platelet function in coronary patients with type II diabetes Cavalca In vivo evaluation of the effect of treatment with folic acid on the metabolic pathway of nitric oxide synthesis Cavalca N-acetylcysteine as a treatment in the iperomocysteinuric patient not responding to folic acid therapy Cavalca Transcriptome analysis in blood leukocytes of patients with coronary artery disease Colombo Association between the BDNF Val66Met polymorphism and coronary artery disease Colombo Circulating microRNAs in atrial fibrillation D'Alessandra Analysis of circulating microRNAs in patients with coronary artery disease D'Alessandra Indices of systemic and cellular activation, modulation of oxidative stress in aortic valve replacement Nava Prevention of atherothrombotic risk Parolari Assessment of the carotid intima-media thickness contribution to the cardiovascular risk. Comparison among different European populations at high and low risk. Tedesco Transcriptomics of antiplatelet resistance Tremoli Antiplatelet effect of aspirin at low doses every 12 hours in patients undergoing coronary artery bypass graft and / or aortic valve replacement using bioprosthesis Tremoli Impact of the measurement of carotid intima-media thickness on cardiovascular risk classification in patients in primary prevention Veglia Evaluation of the flow-mediated dilatation (FMD) of the brachial artery using the lumen area in place of the diameter Veglia Calculation of the minimum amount of measurements needed to correctly estimate the progression of subclinical atherosclerosis Veglia Nutrient-drug interaction: green tea and simvastatin Werba Oral niacin flush. Predictive value of skin tests using methylnicotinate Werba CRITICAL CARDIOLOGY 238 CCM — Scientific Report 2011 — Ongoing research 2012 Influence of ACE genotype on lung diffusion (DLCO) at rest and after intravenous water load in patients with chronic heart failure (CHF) receiving ACE inhibitors Agostoni Treatment of severe heart failure by ultrafiltration Agostoni A multicenter, randomized, double-blind, parallel group, active-controlled study to evaluate the efficacy and safety of both aliskiren monotherapy and aliskiren/enalapril combination therapy compared to enalapril monotherapy, on morbidity and mortality in patients with chronic heart failure (ALISKIREN - CSPP100F2301 - ATMOSPHERE) Agostoni Evaluation of the effects of 4 oral dosages of S 44121 vs placebo on cardiac function and NT-proBPN in patients with chronic heart failure and left ventricular dysfunction not treated with a beta-blocker (CL2 4412-003) Agostoni Evaluation of the effects of 4 oral dosages of S 44121 vs placebo on cardiac function and NT-proBPN in patients with chronic heart failure and left ventricular dysfunction not treated with a beta-blocker (CL2 4412-004) Agostoni CCM — Scientific Report 2011 — Ongoing research 2012 239 240 International registry on cardioversion of atrial fibrillation (RHYTHM-AF) Agostoni INTERVENTIONAL CARDIOLOGY "Sleep and Heart" Italian Multicenter Project (PROMISES) Agostoni Percutaneous mitral repair using Evalve MitralClip Bartorelli Effects of beta 2-receptor blocking on pulmonary function in a human model of acute fluid overload Agostoni Agostoni Clinical evaluation of a new procedure for percutaneous denervation of the renal sympathetic nervous system in patients with hypertension refractory to drug treatment Bartorelli Evaluation of the dead space in patients with chronic heart failure Evaluation of the effects of beta-blocker therapy on exercise tolerance in uncomplicated hypertension Alimento A continuation in the clinical evaluation of the BVS everolimus eluting coronary stent system in the treatment of patients with de novo native coronary artery lesions (ABSORB EXTEND) Bartorelli Reference values of cardiac output during exercise in healthy subjects. Cattadori Bartorelli Psychological assessment and dyastolic dysfunction in hypertension (Paddy study) Fiorentini A randomized comparison of the NEVOTM Sirolimus-eluting coronary stent system using a bioresorbable polymer vs the Everolimus-eluting coronary stent system (XIENCE V/ XIENCE PRIME/PROMUS) using a durable polymer in coronary artery lesions (NEVO II) Clinical and prognostic significance of vitamin D plasma levels in patients with acute coronary syndrome Marenzi Bartorelli Prognostic significance of acute renal failure in course of acute coronary syndrome Marenzi A phase IV pilot study to evaluate kidney measured by neutrophil gelatinase-associated lipocalin (NGAL) as a new bio-marker in patients with normal GFR undergoing percutaneous coronary intervention with IOPAMIDOL injection 370 or IODIXANOL 320 (IOP 116) Prevention of contrast nephropathy in patients affected by renal failure in diuretic therapy and controlled hydration (Renal Guard) Marenzi Bartorelli Impact of different therapeutic approaches in patients with cardiorenal syndrome in course of acute congestive heart failure Marenzi A multicenter, double-blind, randomized trial to determine the clinical benefit and safety of vytorin versus simvastatin monotherapy in high-risk patients with acute coronary syndrome (IMPROVE-IT) Marenzi A prospective, single blind, randomized controlled study to evaluate the safety and effectiveness of the tryton side branch stent™ used in conjunction with a drug-eluting stent compared to side branch balloon angioplasty in conjunction with a drug-eluting stent in the treatment of de novo bifurcation lesions involving the main branch and side branch within the native coronary circulation (TRYTON) Evaluating Xience V in Multi Vessel Disease (EXECUTIVE registry) Bartorelli A multicenter, randomized, double blind, placebo controlled study to evaluate the safety and efficacy of SCH530348 in addition to standard of care in subjects with a history of atherosclerosis disease: thrombin receptor antagonist in secondary prevention of atherothrombotic ischemic events (TRA2P TIMI 50) Marenzi Randomized evaluation of intracoronary nitroprusside vs adenosine after thrombus aspiration during primary PErcutaneous coronary intervention for the prevention of No reflow in Acute Myocardial Infarction (REOPEN-AMI ) Fabbiocchi Marenzi Multicenter registry of the treatment of acute myocardial infarction according to the currently available best practice (OPTIMA) Fabbiocchi Long-term follow-up of management models of antithrombotic therapies in patients with acute coronary syndrome (EPICOR) Safety and efficacy evaluation of short-term treatment with A-2002 in patients with acute coronary syndromes (VISTA 16) Marenzi PROMUSTM ElementTM Everolimus-eluting coronary stent system European post-approval surveillance study . A prospective, open-label, multicenter, observational study with all-comers enrollment (PE-PROVE) Fabbiocchi A randomized, double-blind, placebo controlled, parallel group, multinational trial, to assess the prevention of thrombotic events with ticagrelor compared to placebo on a background of acetyl salicylic acid (ASA) therapy in patients with history of myocardial infarction (PEGASUS-TIMI 54) Marenzi Cangrelor versus standard therapy to achieve optimal management of platetel inhibition (PHOENIX-TMC CAN 10-01) Galli S Marenzi AnGiox in elderly subjects with myocardial infarction (with or without ST-segment elevation) undergoing percutaneous coronary intervention (PCI) in Lombardy, Lombardy AGE-MI Registry. Coordinated by the Regional Registry Study Group LombardIMA - Hippocrates Research Galli S Randomized, double-blind, triple-dummy trial to compare the efficacy of otamixaban with Unfractionated Heparin + eptifibatide, in patients with Unstable angina/Non ST segment Elevation Myocardial infarction scheduled to undergo an early invasive strategy (SEPIA 2 -EFC6204 TAO) Marenzi Myocardial contrast-echocardiography role in the assessment of acute and chronic outcome in PCI and CTO. Comparison with MR angiography by dipyridamole stress Grancini A phase II, randomized, double-blind, parallel-arm, placebo-controlled, with variation of the dose study to evaluate the safety and efficacy of apixaban in patients with recent-onset of acute coronary syndrome (APPRAISE-APIXABAN) Short-term clinical outcome in patients with percutaneous or surgical coronary revascularization combined with valve surgery Lualdi Project to implement adherence to guidelines in the management of acute coronary syndromes during intra-and posthospitalization (BLITZ 4) Marenzi Assessment of myocardial functional recovery after percutaneous reopening of a chronic total occlusion in patients with monovascular coronary artery disease. Role of MR angiography Lualdi Evaluation of early cessation or reduction of cigarette smoking through the use of electronic cigarette used as an adjunct to standard counseling activities (SMOKING) Marenzi Tolerability and safety of the proximal cerebral protection during carotid stenting in patients with intracranial variants of the Willis circle Montorsi Identification of proteomic / proinflammatory and immune biomarkers in patients with acute coronary syndromes at high risk to develop clinical events: genomic and proteomic approaches Marenzi Evaluation of carotid stenosis by CT angiography. Comparison with intravascular carotid assessment by IVUS Montorsi Long-term follow-up of management models of antithrombotic therapies in patients with acute coronary syndrome (EPICOR) Palermo Endovascular treatment of carotid "near-occlusion" Montorsi Using the biomarker copeptin for the early exclusion of a serious condition in patients presenting with symptoms of "acute chest pain." Salvioni A phase III, double blind, randomized, placebo controlled study to evaluate the effects of R04607381 on cardiovascular risk in stable CHD patients with a documented recent acute coronary syndrome (EFFETTI RO 4607381) Salvioni A multicenter, randomized, double-blind, placebo-controlled study to evaluate the safety and efficacy of SCH 530348 in addition to standard of care in subjects with acute coronary syndrome: thrombin receptor antagonist for clinical event reduction in acute coronary syndrome (TRACER ) Salvioni Study of cardiovascular events to evaluate the potential of aleglitazar in reducing cardiovascular risk in patients with Type-2 diabetes mellitus (T2D) and recent episode of acute coronary syndrome (ALECARDIO) Salvioni Steroids In cardiac surgery (SIRS) Parolari Phase III, multicenter, randomized, double-blind, placebo-controlled trial to evaluate the effect of saxagliptin on cardiovascular death , myocardial infarction or ischemic stroke incidence in patients with type 2 diabetes (SAVOR) Salvioni Compassionate therapy with intramyocardial injection of autologous marrow cells in patients with refractory myocardial ischemia Pompilio RE-LY registry on atrial fibrillation (AF): risk factors, treatments and outcomes of patients with atrial fibrillation admitted to the emergency department in multiple regions of the world (RE-LY ) Salvioni Pompilio Randomized, placebo-controlled trial to assess cardiovascular outcomes after treatment with sitagliptin in patients with type 2 diabetes mellitus and inadequate glycemic control (TECOS) Salvioni A double-blind, randomized, placebo-controlled, parallel group study to evaluate the efficacy and safety of four 4 mg doses of XRP0038/NV1FGF at intervals of 2 weeks on the events of amputation or death from any cause in patients with critical ischemia of lower limbs and skin lesions (TAMARIS) Salvioni A prospective, randomized, multicenter, international drug vs placebo to assess the impact of clonidine and acetylsalicylic acid (ASA) in patients undergoing noncardiac surgery at risk for cardiovascular events in the perioperative (POISE 2) Salvi Randomized, placebo-controlled trial to assess cardiovascular outcomes after treatment with exenatide once weekly in patients with diabetes mellitus type 2 ( EXSCEL ) N-acetylcysteine in the prevention of contrast nephropathy in transcatheter aortic prosthesis implantation Sisillo A comparison between prasugrel and clopidogrel in acute coronary syndrome (ACS) subjects with UA/NSTEMI who are medically managed (TRILOGY ACS Study) Salvioni CCM — Scientific Report 2011 — Ongoing research 2012 Correlation among clinical, angiographic and intra-hospital outcomes in myocardial infarction with ST-segment elevation Italian AvantgarDE Dual AntiplateLet Therapy Registry (IDEAL) Ravagnani Trabattoni D CARDIOVASCULAR SURGERY SOURCE Registry: Edwards Sapien Aortic Bioprosthesis European Outcome registry Fusari SOURCE XT Registry: Edwards SAPIEN XT Aortic Bioprothesis Multi-Region Outcome Registry Fusari Omega-3 Fatty Acids for Prevention of Post-Operative Atrial Fibrillation (OPERA) Parolari TM CCM — Scientific Report 2011 — Ongoing research 2012 241 Relationship between lipoprotein profile, plasma thiol level of inflammatory markers and carotid atherosclerosis. Identification of plasma biomarkers of cardiovascular disease Spirito Expression of molecules involved in athero-thrombotic and aneurysmal process in infrarenal aortic perivascular adipose tissue Spirito Endovascular treatment of steno-occlusions in the SFA by Zilver PTX stent Trabattoni P Acute type A dissection: emergency surgical treatment combined with E-XL Aortic Stent Trabattoni P Hybrid treatment of aortic arch aneurysms Trabattoni P Modification of peri-and postoperative right ventricular function in mitral valve plastic: influence of the surgical approach and the mode of myocardial protection Zanobini Electrophysiology Coronary atherosclerosis in outlier subjects: protective and individual risk factor evaluation (GISSI Outliers CAPIRE ) Andreini Pathophysiological determinants of mitral annulus tissue Doppler systolic velocity obtained by high resolution echocardiography Barbier Accurate real-time 3D echocardiography in the localization of trans esophageal mitral valve prolapse: comparison between visual method and with dedicated software Pepi Quantitative intraoperative evaluation of mitral valve apparatus pre-and post- annuloplasty intervention Pepi New techniques of morphofunctional evaluation of the tricuspid ring and valve and right ventricle by reconstruction from MRI and 3D echocardiographic images Pepi Role of multidetector CT (MDCT) in evaluation of patients undergoing percutaneous aortic valve implantation (TAVI) Pontone Feasibility and diagnostic accuracy of ultra low dose'''' multidetector CT in the evaluation of coronary artery disease Pontone New anatomical parameters of the left atrium as predictors of atrial fibrillation Pontone Role of low-dose MDCT in the preoperative evaluation of patients with mitral valve prolapse Pontone Clinical study on the use of a electrophysiology low flow irrigation electrocatheter for the ablation of ventricular tachycardia Carbucicchio Pacemapping techniques for identification of the ablation site in patients with ventricular arrhythmias: validation and utility of a new system of mathematical analysis (PAcing SOftware). Carbucicchio Comparison between 64-slice cardiac CT and stress echo in the diagnosis of significant coronary artery disease Pontone Endomyocardial biopsy via transeptal puncture in patients undergoing atrial fibrillation ablation. Searching for new biomarkers using analysis of tissue microRNAs Casella Role of Magnetic Resonance Imaging (MRI) in assessing aortic annulus in patients undergoing percutaneous aortic valve implantation (TAVI). Pontone Mapping and ablation of ventricular extrasystoles: usefulness of the automatic algorithm "Paso" implemented in the mapping system CARTO (MAE-Paso) Casella 3D transesophageal assessment of right ventricular size and function in the operating room Tamborini Near zerO fluoroscopic exPosure during catheter ablAtion of supRavenTricular arrhYthmias (NO-PARTY) Casella 3D assessment of left atrial size and function pre-and post-plastic mitral surgery. Tamborini Percutaneous implantation of aortic valve prosthesis: 3D transesophageal echocardiography usefulness Tamborini Impact of percutaneous aortic valve replacement (TAVI) on left ventricular systolic and diastolic function : echocardiographic long-term follow-up Tamborini Morphological and electrophysiological characteristics of myocardial substrate associated with increased arrhythmic risk in patients with dilated cardiomyopathy (EMOSIDD) Dello Russo Usefulness of cardiac MRI in the identification of intraventricular desynchronization area in patients undergoing ventricular resynchronization therapy Dello Russo Substrate in Heart failure And effectiveness of Resynchronization Therapy by EnSite Array system (SHARE-M) Dello Russo Evaluation of cardiac output by cardiopulmonary exercise testing with non-invasive measurement in patients with chronic atrial fibrillation undergoing catheter ablation Fassini Monitoring after catheter ablation of atrial fibrillation by implantation of implantable recorder (loop recorder) Moltrasio Massimo Interference between the modern implantable cardiac devices and instrumentation used in the dental setting. An in vivo study Moltrasio Massimo Atrial fibrillation ablation registry Moltrasio Massimo Monitoring resynchronization in cardiac patients (MORE CARE) Moltrasio Massimo Genetic polymorphism and incidence of intra-atrial thrombosis in patients with permanent AF / chronic despite adequate oral anticoagulation Riva Assessing the usefulness of the delayed-enhancement MRI in determining the degree of atrial fibrosis and its prognostic correlation with the medium / long term efficacy of chronic AF transcatheter ablation Riva Identification of the levels of autonomy of patients undergoing implantation of mono and bicameral pacemaker Tondo Role of endomyocardial biopsy guided by electroanatomic mapping in the definition of the arrhythmic substrate in patients with ventricular arrhythmias without apparent organic heart disease or uncertain diagnostic tests Tondo Endoscopic Guided Ablation and Voyage mapping (IRIS) Tondo A prospective, randomized, milticenter, interventional study designed to evaluate the safety and efficacy of percutaneous ablation catheter TactiCath for the treatment of symptomatic paroxysmal atrial fibrillation using an irrigated catheter for radiofrequency ablation with full recognition of the contact force (ToccaStar) Tondo Clinical WoRkflow Study for the EValuation Of the Multi-ELectrode PUlmonary Vein Isolation System for the Treatment of Paroxysmal AtrIal FibrillatiON (REVOLUTION) Tondo Post-market clinical study of the CardioFocus endoscopic ablation system-adaptive contact (CF-EAS-AC) Tondo-Dello Russo CARDIOVASCULAR IMAGING 242 Additional clinical role of 64 slice cardiac MDCT in the visualization of anatomical variants and of coronary anomalies Andreini Feasibility and diagnostic accuracy of MDCT in the evaluation of coronary circulation in diabetic patients with suspected coronary artery disease Andreini Feasibility and diagnostic accuracy of multidetector low-dose CT in the evaluation of coronary stents patency Andreini Prognostic role of multidetector CT in patients undergoing coronary artery bypass graft Andreini Comparison between nuclear magnetic resonance (NMR) and two-dimensional echocardiography in the quantification of mitral regurgitation in mitral valve prolapse Andreini CCM — Scientific Report 2011 — Ongoing research 2012 CCM — Scientific Report 2011 — Ongoing research 2012 243 Ongoing Grants in 2011 Age.na.s •Training of pharmacists: estimation of cardiovascular risk and approach to critical situations European Commission •IMPROVE •Role of cyclophilin A in bone marrow vascular progenitor cell mobilization and recruitment in the angiogenic response to ischemia - CAPI •Nucleolar-dependent secretion of microRNA in a model of doxorubicin and trastuzumab cardiomyopathy - NUMIRDT Fondazione Monzino •Development of engineered cardiac valves •Laboratory of experimental surgery: cardiovascular regenerative therapy •New pathogenetic mechanisms of acute coronary syndromes •Study of the pathogenic mechanisms of heart failure during emotional stress Fondazione Veronesi •The circulating transcriptome in coronary artery disease: a next generation sequencing approach Ministero della Salute Ricerca Corrente •Absorption of the glycosaminoglycans (GAGs) into saphenous vein wall after their oral administration •Analysis of the functional role of pentraxin 3 in endothelial cells through an integrated approach of proteomics and gene silencing •Analysis of the functional role of tissue factor in cardiomyocytes through an integrated approach of proteomics and gene silencing •Analysis of transcriptional profiles associated to brain damage in spontaneously hypertensive stroke prone (SHRSP) rats •Aortic valve with minimally-invasive implantation •Assessing oxidative stress in patients with carotid stenosis underwent surgical treatment and / or carotid stenting •Assessment of the effectiveness of a medium / long term complex multistep strategy in the transcatheter ablation of chronic AF •Brachial artery diameter: a new marker of atherosclerosis? •CABG, genomics, perioperative changes in hemostasis and inflammation and clinical outcomes at follow-up. •Carotid atherosclerotic plaque: characterization by imaging, biochemical and histopathological techniques •Caveolin-rich membrane microdomains and Tissue Factor modulation by protease receptors (PARS): role of cholesterol biosynthesis inhibitors •Cell therapy of heart failure and ischemic heart injury •Characterization by MRI techniques of heart ischemia in ApoE KO mice •Characterization of cells derived from cardiac mesenchyme: epigenetic and functional studies, stem cell reprogramming •Characterization of human carotid plaques by imaging techniques and histopathology 244 CCM — Scientific Report 2011 — Ongoing research 2012 •Characterization of the epigenetic role of nitric oxide in aging and cellular senescence •Clinical evaluation of safety and efficacy of a new system of hemostasis (QuikClot® Interventional) after diagnostic percutaneous coronary or interventional procedures •Correlation between platelet and megakaryocyte trascriptome in CAD patients •Development of a procedure for “decellularisation” and cryo-preservation of human pericardial patches in order to engineer cardiovascular tissue •Development of innovative diagnostic systems for atherosclerotic disease: ANN-IDA study •Development of methods based on mass spectrometry for the absolute quantitative analysis of proteins in biological samples •Development of murine model of dilated cardiomyopathy induced by doxorubicin and trastuzumab •Echocardiographic and histological study of the influence of aging on left atrial function in mice •Effect of cigarette smoke in the modulation of endothelial dysfunction •Effect of drugs in drug-eluting stents on endothelial function and oxidative stress •Effectiveness of nitric oxide and Histone Deacetylases inhibitors in dystrophic cardiomyopathy: identification of common targets using a proteomic approach •Endothelial cell secretoma •Endovascular exclusion of aneurysms of the thoraco-abdominal aorta by fenestrated endograft: advantages of the radiology suite in elective and emergency implantation •Engineered tissues: cryopreserved valves cellularized by autologous cells of the recipient. •Epigenetic modifications and impaired endothelialization of circulating endothelial progenitor cells in normal subjects and patients at risk •Epigenetic role of chronic electrical stimulation in cardiac cells •Evaluation of the platelet activation state following stent placement in the carotid and / or iliac-femoral artery. Observational study •Evaluation of the hemostatic system in the mouse COX-2 knockout •Evaluation of the molecular mechanisms involved in the stabilization of platelet mRNA •Functional adaptation of the stem cell population of the saphenous vein (SVPs) as a factor predisposing to the development of restenosis in coronary artery bypass grafting •Genomic and proteomic expression profile of diabetic patients affected by platelet coronary syndromes •Glycosaminoglycan and proteoglycan determinations in human aortic valves in normal and pathological conditions. •GMP development of resident cardiac progenitors •GPR17 purinergic receptor expression in stem cells residing in the heart •Identification of human macrophage markers associated to the phenotype 5/1000 •Identification of the molecular targets of aspirin by a proteomic approach •Identification of the role of the new purinergic receptor GPR17 in cardiomyocytes using a proteomic approach •Impact of the BDNF Val66Met polymorphism on the hemostatic system: possible differences between the sexes •Inflammation and cerebral ischemia •Influence of dyslipidemia on left atrial size and compliance in subjects with isolated hypercholesterolemia •Interactions between stem cells and biopolymers using’’ high throughput’’ systems, towards the engineering of artificial stem cell niches for cardiovascular tissue bio-engineering •Mecki score (Metabolic, Exercise, Cardiac, Kidney Index) for the identification of cardiovascular risk in patients with heart failure •MicroRNAs and aging •Minimally invasive aortic and mitral valve surgery •Mitochondrial proteome of cardiac cells HL-1 •Mitral valve disease: genetic and phenotypic markers predictive of progression of the disease: systematic review of the literature •Modulation of endothelial prostanoids by cigarette smoke in association with IL-1 beta •New markers of vascular imaging as predictors of vascular events in a European population of patients at high risk (new projects based on the IMPROVE study) •New model of left atrial function in mice •Optimization of time / temperature in the decontamination of cardiovascular tissues with BASE.128 •Pharmacological control of cerebral ischaemia •Plasma fatty acids and nutrition in patients with overt coronary artery disease CCM — Scientific Report 2011 — Ongoing research 2012 245 •Platelet function in cardiac patients with chronic renal failure •Possible role of brain-derived neurotrophic factor (BDNF) in the thrombosis •Precursors of endothelial and smooth muscle cells in the abdominal aortic aneurysm: role of Cyclofillin A and microRNAs modulated by aging •Predictors of peri-operative renal injury after adult cardiac surgery: role of the pre-, intra-and postoperative variables and of the extracorporeal circulation management •Proteomics of atherosclerotic plaque •Proteomics of C. elegans and effects of the silencing of the gene R53.1, the human ortholog of the gene FLAD1 •Proteomics of human heart valves •Proteomics of plasma lipoproteins: identification of new associated molecules and clinical implications •Proteomics of procoagulant microparticles •Regeneration in adult zebrafish heart as a model for repair of cardiac ischemia •Registry and Biobank of aortic valve disease •Registry and Biobank of mitral valve disease •Registry and Biobank of thoracic and abdominal aortic aneurysms and acute aortic syndromes •Regulation of the alveolar capillary membrane function: is protein SP-B a useful marker? •Regulation of the biosynthesis of Dickkopf-1 (Dkk-1) by statins in human endothelial cells •Regulation of the pentraxin 3 biosynthesis by statins in human endothelial cells •Relationship between platelet reactivity index and risk of adverse cardiovascular events in patients with acute coronary syndrome treated with coronary angioplasty •Role of cyclooxygenase-2 (COX-2) metabolites in the regulation of Tissue Factor (TF) induced by cigarette smoke •Role of cyclooxygenase-2 in a mouse model of thrombosis •Role of melanocortins in the restenosis and stent thrombosis prevention •Study of the role of RAGE and HMGB1 in cardiovascular aging and development of cardiac fibrosis •Surgical techniques to support electrophysiological procedures •TF-dependent procoagulant contribution in leukocytes and platelets of patients with CAD •The sum of early family aggregation for vascular disease in different districts and for risk factors as a novel risk factor for atherosclerosis •Thrombosis of drug-eluting stent •Use of antithrombotics in atrial fibrillation (ATA - AF) Ricerca Finalizzata •Breathing disorders in heart failure: high altitude hypoxia as a model to define diagnostic tools, therapeutic strategies •Identification of proteomic/proinflammatory and immune biomarkers in patients with acute coronary syndromes at high risk to develop clinical events: genomic and proteomic approaches •Insulin resistance and coronary disease: insights into inflammation, thrombosis and metabolic syndromes •Role of longevity genes P66SH/SIR1 in insulin-resistance, diabetes and cardiovascular diseases •Implementing brain repair in stroke via the exploiment of adult neurogenesis and gliogenesis: focus on the cross-talk between microglial and endogenous precursor cells •MicroRNA bioengeneering of human cardiac mesenchymal cells and heart regeneration Progetti interni •Cardiovascular Tissue Bank in Lombardia •Clinical audit- Heart Surgery •Clinical audit-Cardiology •Patient analysis and tracking system data form Regione Lombardia •microRNA as new early markers of acute myocardial ischemia •Echocardiographic imaging of the left atrium as a marker of cardiovascular events •Setting up diagnostic and therapeutic pathways with the aid of telemedicine to identify mechanisms for the presentation and development of atrial fibrillation. A prospective randomized multicenter study (PER.DI.FIA.TO) 246 CCM — Scientific Report 2011 — Ongoing research 2012 CCM — Scientific Report 2011 — Ongoing research 2012 247 Seminars, conferences and courses 2011 Seminars April 19 - Salvatore Cuzzocrea (Messina) “Strategies to reduce I/R injury” April 29 - Germano Ferrari (Milano) “Best practices in technology transfer: from intellectual property protection to market” May 24 - Nicholas W. Shworak (Lebanon, NH, USA) “A novel anti-inflammatory pathway of the blood vessel wall” May 31 - Giuseppe Gaipa (Monza) “Single cell phosphoflow analysis in haematological malignancies: methods and applications” June 07 - Silvia Soddu (Roma) “HIPK2: dall’attivazione di p53 in risposta al danno al DNA alla citochinesi” June 14 - Marco Bianchi (Milano) “HMGB1, inflammation and tissue regeneration” June 30 - Lina Badimon (Barcellona) “Atherosclerotic plaque complications: plaque angiogenesis” July 12 - Bianca Rocca (Roma) “Variability in the responsiveness to low dose aspirin: pharmacological and disease-related mechanisms” September 20 - Massimiliano Gnecchi (Pavia) “Use of mesenchymal stem cells to repair infarcted hearts” September 27 - Andrea Urbani (Roma) “Clinical proteomics strategies and investigations: a perspective” 248 CCM — Scientific Report 2011 — Ongoing research 2012 October 11 - Elisabetta Cerbai (Firenze) “Alterazioni elettrofisiologiche cellulari nell’ipertrofia e insufficienza cardiaca umana: basi molecolari e prospettive farmacologiche” October 25 - Huei-Sheng Vincent Chen (La Jolla) “Modeling inherited cardiac diseases with patientspecific iPScells” November 22 - Angelo Scuteri (Roma) “L’ importanza del fenotipo per valorizzare i risultati della ricerca di base. Il modello della sindrome metabolica” November 30 - Mauro Giacca (Trieste) “How can we mend a broken heart” (Bee Gees, 1971): searching for genes that induce myocardial protection or repair by in vivo gene transfer using AAV vectors”” September 24 - Cesare Fiorentini, Elena Tremoli “Giornata mondiale per il cuore 2011” November 16 - Piergiuseppe Agostoni “Beta-bloccanti e scompenso:come scegliere” November 03-04 - Elena Tremoli “Aterotrombosi: dalla ricerca di base alla clinica” V Convegno monotematico della SIF November 21-22 - Claudio Tondo “Biopsia endomiocardica per elettrofisiologi” November 16 - Piero Montorsi “ 3° Audit Stenting carotideo” November 21-22 - Piero Montorsi “19° Carotiday” Corso di stenting carotideo December 14 - Rita Spirito “Il piede vascolare: percorso diagnostico-terapeutico” November 21-23 - Alessandro Lualdi “Corso teorico applicativo di Cardiologia Interventistica” Courses March 21-22- Piero Montorsi “17° Carotiday” Corso di stenting carotideo Feb-Mar-Apr-May-Jun - Marco Agrifoglio “Corso di perfezionamento in Ecocolordoppler Vascolare” Jan-Feb-Apr-Jun-Oct-Nov - Claudio Tondo “Tecnica della puntura transettale e trattamento della fibrillazione atriale mediante crioablazione” April 01 - Stefano Galli, Piero Montorsi, Paolo Ravagnani “Focus IVUS Advanced” May 9-10 - Piergiuseppe Agostoni: “Il test da sforzo cardiopolmonare (CPET): basi fisiologiche, indicazioni e interpretazione” May 27 - Stefano Galli, Piero Montorsi, Paolo Ravagnani “Focus IVUS Basic” September 13-15 - Mauro Pepi, Paolo Barbier “Corso base di ecocardiografia” Conferences March 03 - Elena Tremoli “Il cuore del Monzino per le donne” March 30 - Paolo Biglioli, Francesco Alamanni, Cesare Fiorentini “Live Cardiac Surgery. Treatment of heart failure” September 26-28 - Claudio Tondo “Corso teoricopratico sulle diverse tecniche di puntura transettale per elettrofisiologi” October 24 - Paolo Barbier “Rigurgito mitralico: dalla quantificazione ecodoppler all’analisi morfologica 3D nella routine diagnostica” May 09 - Paolo Biglioli. Cesare Fiorentini “ Audit Day 2011” October 24-25 - Corrado Carbucicchio, Claudio Tondo “Mappaggio e ablazione transcatetere di aritmie ventricolari” June 08 - Daniela Trabattoni “Forame Ovale Pervio: quando, come, perché intervenire” November 7-8 - Corrado Carbucicchio, Claudio Tondo “Puntura pericardica e mappaggio epicardico” June 10 - Paolo Ravagnani “La cardiopatia ischemica nel terzo millennio: è tempo per una riflessione” November 15-17 - Mauro Pepi, Paolo Barbier “Corso avanzato di ecocardiografia” CCM — Scientific Report 2011 — Ongoing research 2012 249 Centro Cardiologico Monzino Istituto di Ricovero e Cura a Carattere Scientifico Via Parea 4 20138 Milano T +39 02 580021 F +39 02 504667 W www.cardiologicomonzino.it Si cura meglio dove si fa ricerca