Robert L Ferris1, Yael Flamand2, F Christopher Holsinger3, Gregory S Weinstein4, Harry Quon5, Ranee Mehra6, Joaquin J Garcia7, Michael L Hinni8, Neil D Gross9, Erich M Sturgis9, Umamaheswar Duvvuri10, Eduardo Méndez11, John A Ridge12, J Scott Magnuson13, Kerry A Higgins14, Mihir R Patel15, Russel B Smith16, Daniel W Karakla17, Michael E Kupferman9, James P Malone18, Benjamin L Judson19, Jeremy Richmon20, Jay O Boyle21, Rodrigo Bayon22, Bert W O'Malley4, Enver Ozer23, Giovana R Thomas24, Wayne M Koch5, R Bryan Bell25, Nabil F Saba15, Shuli Li2, Elin R Sigurdson12, Barbara Burtness19. 1. UPMC Hillman Cancer Center, Pittsburgh, PA, United States. Electronic address: Ferrisrl@upmc.edu. 2. Dana Farber Cancer Institute-ECOG-ACRIN Biostatistics Center, Boston, MA, United States. 3. Stanford University, Palo Alto, CA, United States. 4. University of Pennsylvania, Philadelphia, PA, United States. 5. Johns Hopkins University, Baltimore, MD, United States. 6. University of Maryland, Baltimore, MD, United States. 7. Mayo Clinic, Rochester, MN, United States. 8. Mayo Clinic in Arizona, Phoenix, AZ, United States. 9. The University of Texas, M.D. Anderson Cancer Center, Houston, TX, United States. 10. UPMC Hillman Cancer Center, Pittsburgh, PA, United States. 11. University of Washington, Seattle, WA, United States. 12. Fox Chase Cancer Center, Philadelphia, PA, United States. 13. Florida Hospital Orlando, Celebration, FL, United States. 14. ECOG-ACRIN Cancer Research Group, Boston, MA, United States. 15. Winship Cancer Institute at Emory University, Atlanta, GA, United States. 16. University of Nebraska, Omaha, NE, United States. 17. Sentara Norfolk General Hospital, Norfolk, VA, United States. 18. UPMC Pinnacle Cancer Center, Harrisburg, PA, United States. 19. Yale School of Medicine and Yale Cancer Center, New Haven, CT, United States. 20. Massachusetts Eye and Ear, Harvard University, Boston, MA, United States. 21. Memorial Sloan Kettering Cancer Center, New York, NY, United States. 22. University of Iowa, Iowa City, IA, United States. 23. The Ohio State University, Columbus, OH, United States. 24. University of Miami Leonard Miller School of Medicine, Miami, FL, United States. 25. Providence Cancer Institute, Portland, OR, United States.
Abstract
PURPOSE: Understanding the role of transoral surgery in oropharyngeal cancer (OPC) requires prospective, randomized multi-institutional data. Meticulous evaluation of surgeon expertise and surgical quality assurance (QA) will be critical to the validity of such trials. We describe a novel surgeon credentialing and QA process developed to support the ECOG-ACRIN Cancer Research Group E3311 (E3311) and report outcomes related to QA. PATIENTS AND METHODS: E3311 was a phase II randomized clinical trial of transoral surgery followed by low- or standard-dose, risk-adjusted post-operative therapy with stage III-IVa (AJCC 7th edition) HPV-associated OPC. In order to be credentialed to accrue to this trial, surgeons were required to demonstrate active hospital credentials and technique-specific surgical expertise with ≥20 cases of transoral resection for OPC. In addition, 10 paired operative and surgical pathology reports from the preceding 24 months were reviewed by an expert panel. Ongoing QA required <10% rate of positive margins, low oropharyngeal bleeding rates, and accrual of at least one patient per 12 months. Otherwise surgeons were placed on hold and not permitted to accrue until re-credentialed using a new series of transoral resections. RESULTS: 120 surgeons trained in transoral minimally invasive surgery applied for credentialing for E3311 and after peer-review, 87 (73%) were approved from 59 centers. During QA on E3311, positive final pathologic margins were reported in 19 (3.8%) patients. Grade III/IV and grade V oropharyngeal bleeding was reported in 29 (5.9%) and 1 (0.2%) of patients. CONCLUSIONS: We provide proof of concept that a comprehensive credentialing process can support multicenter transoral head and neck surgical oncology trials, with low incidence of positive margins and *grade III/V oropharyngeal bleeding.
PURPOSE: Understanding the role of transoral surgery in oropharyngeal cancer (OPC) requires prospective, randomized multi-institutional data. Meticulous evaluation of surgeon expertise and surgical quality assurance (QA) will be critical to the validity of such trials. We describe a novel surgeon credentialing and QA process developed to support the ECOG-ACRIN Cancer Research Group E3311 (E3311) and report outcomes related to QA. PATIENTS AND METHODS: E3311 was a phase II randomized clinical trial of transoral surgery followed by low- or standard-dose, risk-adjusted post-operative therapy with stage III-IVa (AJCC 7th edition) HPV-associated OPC. In order to be credentialed to accrue to this trial, surgeons were required to demonstrate active hospital credentials and technique-specific surgical expertise with ≥20 cases of transoral resection for OPC. In addition, 10 paired operative and surgical pathology reports from the preceding 24 months were reviewed by an expert panel. Ongoing QA required <10% rate of positive margins, low oropharyngeal bleeding rates, and accrual of at least one patient per 12 months. Otherwise surgeons were placed on hold and not permitted to accrue until re-credentialed using a new series of transoral resections. RESULTS: 120 surgeons trained in transoral minimally invasive surgery applied for credentialing for E3311 and after peer-review, 87 (73%) were approved from 59 centers. During QA on E3311, positive final pathologic margins were reported in 19 (3.8%) patients. Grade III/IV and grade V oropharyngeal bleeding was reported in 29 (5.9%) and 1 (0.2%) of patients. CONCLUSIONS: We provide proof of concept that a comprehensive credentialing process can support multicenter transoral head and neck surgical oncology trials, with low incidence of positive margins and *grade III/V oropharyngeal bleeding.
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