Definitions and Clinical Trial Design Principles for Coronary Artery Chronic Total Occlusion Therapies: CTO-ARC Consensus Recommendations

Author:

Ybarra Luiz F.1ORCID,Rinfret Stéphane2ORCID,Brilakis Emmanouil S.3ORCID,Karmpaliotis Dimitri45,Azzalini Lorenzo6ORCID,Grantham J. Aaron7,Kandzari David E.8ORCID,Mashayekhi Kambis9ORCID,Spratt James C.10ORCID,Wijeysundera Harindra C.11ORCID,Ali Ziad A.45ORCID,Buller Christopher E.12,Carlino Mauro13,Cohen David J.14ORCID,Cutlip Donald E.15ORCID,De Martini Tony16,Di Mario Carlo17,Farb Andrew1819,Finn Aloke V.20ORCID,Galassi Alfredo R.21ORCID,Gibson C. Michael22,Hanratty Colm23,Hill Jonathan M.24,Jaffer Farouc A.25ORCID,Krucoff Mitchell W.26,Lombardi William L.27,Maehara Akiko45,Magee P.F. Adrian20,Mehran Roxana28ORCID,Moses Jeffrey W.45,Nicholson William J.29,Onuma Yoshinobu3031ORCID,Sianos Georgios32,Sumitsuji Satoru33,Tsuchikane Etsuo34,Virmani Renu18ORCID,Walsh Simon J.35ORCID,Werner Gerald S.ORCID,Yamane Masahisa36,Stone Gregg W.528ORCID,Rinfret Stéphane,Stone Gregg W.ORCID,

Affiliation:

1. London Health Sciences Centre, Schulich School of Medicine and Dentistry, Western University, Ontario, Canada (L.F.Y.).

2. McGill University Health Centre, McGill University, Montreal, Quebec, Canada (S.R.).

3. Minneapolis Heart Institute and Minneapolis Heart Institute Foundation, Abbott Northwestern Hospital, MN (E.S.B.).

4. New York–Presbyterian Hospital/Columbia University Medical Center, NY (D.K., Z.A.A., A.M., J.W.M.).

5. The Cardiovascular Research Foundation, New York, NY (D.K., A.M., Z.A.A., J.W.M., G.W.S.).

6. Cardiac Catheterization Laboratory, Mount Sinai Hospital, New York, NY (L.A.).

7. Saint Luke’s Mid America Heart Institute, Kansas City, MO (J.A.G.).

8. Piedmont Heart Institute, Atlanta, GA (D.E.K.).

9. Department of Cardiology and Angiology II University Heart Center (K.M.), Freiburg, Bad Krozingen, Germany.

10. St George’s University Hospital NHS Trust, London, United Kingdom (J.C.S.).

11. Schulich Heart Center, Sunnybrook Research Institute, and Institute for Clinical Evaluative Sciences, Sunnybrook Health Sciences Centre, and Institute for Health Policy, Management, and Evaluation (H.C.W.), University of Toronto, Ontario, Canada.

12. St Michael’s Hospital, Toronto, Ontario, Canada (C.E.B.).

13. Interventional Cardiology Unit, IRCCS San Raffaele Scientific Institute, Milan, Italy (M.C.).

14. Baim Institute for Clinical Research, Boston, MA (D.J.C., C.M.G.).

15. University of Missouri–Kansas City (D.E.C.).

16. Southern Illinois University School of Medicine, Memorial Medical Center, Springfield, IL (T.D.M.).

17. Structural Interventional Cardiology, Careggi University Hospital, Florence, Italy (C.D.M.).

18. Department of Cardiovascular Pathology, CVPath Institute, Gaithersburg, MD (A.F., R.V.).

19. School of Medicine, University of Maryland, Baltimore (A.F.).

20. US Food and Drug Administration, Silver Spring, MD (A.V.F., P.F.A.M.).

21. Cardiology, Department of PROMISE, University of Palermo, Italy (A.R.G.).

22. Division of Cardiology, Department of Medicine, Beth Israel Deaconess Medical Center, Harvard Medical School, Boston, MA (D.J.C., C.M.G.).

23. Belfast Health and Social Care Trust, United Kingdom (C.H.).

24. Royal Brompton Hospital, London, United Kingdom (J.M.H.).

25. Cardiology Division, Massachusetts General Hospital, Boston (F.A.J.).

26. Duke Clinical Research Institute and Duke University Medical Center, Durham, NC (M.W.K.).

27. University of Washington, Seattle (W.L.L.).

28. Zena and Michael A. Wiener Cardiovascular Institute, Icahn School of Medicine at Mount Sinai, New York, NY (R.M., G.W.S.).

29. WellSpan Health System, York, PA (W.J.N.).

30. Cardialysis Clinical Trials Management and Core Laboratories, Rotterdam, the Netherlands (Y.O.).

31. Department of Cardiology, National University of Ireland Galway, United Kingdom (Y.O.).

32. AHEPA University Hospital, Thessaloniki, Greece (G.S.).

33. Division of Cardiology for International Education and Research, Osaka University Graduate School of Medicine, Suita, Japan (S.S.).

34. Toyohashi Heart Center, Aichi, Japan (E.T.).

35. Belfast Health and Social Care Trust, United Kingdom. Medizinische Klinik I Klinikum Darmstadt GmbH, Germany (S.J.W.).

36. Saitama-Sekishinkai Hospital, Sayama, Japan (M.Y.).

Abstract

Over the past 2 decades, chronic total occlusion (CTO) percutaneous coronary intervention has developed into its own subspecialty of interventional cardiology. Dedicated terminology, techniques, devices, courses, and training programs have enabled progressive advancements. However, only a few randomized trials have been performed to evaluate the safety and efficacy of CTO percutaneous coronary intervention. Moreover, several published observational studies have shown conflicting data. Part of the paucity of clinical data stems from the fact that prior studies have been suboptimally designed and performed. The absence of standardized end points and the discrepancy in definitions also prevent consistency and uniform interpretability of reported results in CTO intervention. To standardize the field, we therefore assembled a broad consortium comprising academicians, practicing physicians, researchers, medical society representatives, and regulators (US Food and Drug Administration) to develop methods, end points, biomarkers, parameters, data, materials, processes, procedures, evaluations, tools, and techniques for CTO interventions. This article summarizes the effort and is organized into 3 sections: key elements and procedural definitions, end point definitions, and clinical trial design principles. The Chronic Total Occlusion Academic Research Consortium is a first step toward improved comparability and interpretability of study results, supplying an increasingly growing body of CTO percutaneous coronary intervention evidence.

Publisher

Ovid Technologies (Wolters Kluwer Health)

Subject

Physiology (medical),Cardiology and Cardiovascular Medicine

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