Germline mutations in penetrant cancer predisposition genes are rare in men with prostate cancer selecting active surveillance

Lauren Brady; Lisa F. Newcomb; Kehao Zhu; Yingye Zheng; Hilary Boyer; Navonil De Sarkar; Jesse K. McKenney; James D. Brooks; Peter R. Carroll; Atreya Dash; William J. Ellis; Christopher P. Filson; Martin E. Gleave; Michael A. Liss; Frances Martin; Todd M. Morgan; Ian M. Thompson; Andrew A. Wagner; Colin C. Pritchard; Daniel W. Lin; Peter S. Nelson

doi:10.1002/cam4.4778

Cancer Medicine (Nov 2022)

Germline mutations in penetrant cancer predisposition genes are rare in men with prostate cancer selecting active surveillance

Lauren Brady,
Lisa F. Newcomb,
Kehao Zhu,
Yingye Zheng,
Hilary Boyer,
Navonil De Sarkar,
Jesse K. McKenney,
James D. Brooks,
Peter R. Carroll,
Atreya Dash,
William J. Ellis,
Christopher P. Filson,
Martin E. Gleave,
Michael A. Liss,
Frances Martin,
Todd M. Morgan,
Ian M. Thompson,
Andrew A. Wagner,
Colin C. Pritchard,
Daniel W. Lin,
Peter S. Nelson

Affiliations

Lauren Brady: Division of Human Biology Fred Hutchinson Cancer Center Seattle Washington USA
Lisa F. Newcomb: Division of Public Health Sciences Fred Hutchinson Cancer Center Seattle Washington USA
Kehao Zhu: Division of Public Health Sciences Fred Hutchinson Cancer Center Seattle Washington USA
Yingye Zheng: Division of Public Health Sciences Fred Hutchinson Cancer Center Seattle Washington USA
Hilary Boyer: Division of Public Health Sciences Fred Hutchinson Cancer Center Seattle Washington USA
Navonil De Sarkar: Division of Human Biology Fred Hutchinson Cancer Center Seattle Washington USA
Jesse K. McKenney: Robert J. Tomsich Pathology and Laboratory Medicine Institute Cleveland Clinic Cleveland Ohio USA
James D. Brooks: Department of Urology Stanford University Stanford California USA
Peter R. Carroll: Department of Urology University of California San Francisco California USA
Atreya Dash: VA Puget Sound Health Care Systems Seattle WA USA
William J. Ellis: Department of Urology University of Washington Seattle Washington USA
Christopher P. Filson: Department of Urology Emory University School of Medicine Atlanta Georgia USA
Martin E. Gleave: Department of Urologic Sciences University of British Columbia Vancouver British Columbia Canada
Michael A. Liss: Department of Urology University of Texas Health Sciences Center San Antonio Texas USA
Frances Martin: Department of Urology Eastern Virginia Medical School Virginia Beach Virginia USA
Todd M. Morgan: Department of Urology University of Michigan Ann Arbor Michigan USA
Ian M. Thompson: CHRISTUS Medical Center Hospital San Antonio Texas USA
Andrew A. Wagner: Division of Urology Beth Israel Deaconess Medical Center Boston Massachusetts USA
Colin C. Pritchard: Department of Laboratory Medicine and Pathology University of Washington Seattle WA USA
Daniel W. Lin: Division of Public Health Sciences Fred Hutchinson Cancer Center Seattle Washington USA
Peter S. Nelson: Division of Human Biology Fred Hutchinson Cancer Center Seattle Washington USA

DOI: https://doi.org/10.1002/cam4.4778
Journal volume & issue: Vol. 11, no. 22
pp. 4332 – 4340

Abstract

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Abstract Background Pathogenic germline mutations in several rare penetrant cancer predisposition genes are associated with an increased risk of aggressive prostate cancer (PC). Our objectives were to determine the prevalence of pathogenic germline mutations in men with low‐risk PC on active surveillance, and assess whether pathogenic germline mutations associate with grade reclassification or adverse pathology, recurrence, or metastases, in men treated after initial surveillance. Methods Men prospectively enrolled in the Canary Prostate Active Surveillance Study (PASS) were retrospectively sampled for the study. Germline DNA was sequenced utilizing a hereditary cancer gene panel. Mutations were classified according to the American College of Clinical Genetics and Genomics' guidelines. The association of pathogenic germline mutations with grade reclassification and adverse characteristics was evaluated by weighted Cox proportional hazards modeling and conditional logistic regression, respectively. Results Overall, 29 of 437 (6.6%) study participants harbored a pathogenic germline mutation of which 19 occurred in a gene involved in DNA repair (4.3%). Eight participants (1.8%) had pathogenic germline mutations in three genes associated with aggressive PC: ATM, BRCA1, and BRCA2. The presence of pathogenic germline mutations in DNA repair genes did not associate with adverse characteristics (univariate analysis HR = 0.87, 95% CI: 0.36–2.06, p = 0.7). The carrier rates of pathogenic germline mutations in ATM, BRCA1, and BRCA2did not differ in men with or without grade reclassification (1.9% vs. 1.8%). Conclusion The frequency of pathogenic germline mutations in penetrant cancer predisposition genes is extremely low in men with PC undergoing active surveillance and pathogenic germline mutations had no apparent association with grade reclassification or adverse characteristics.

Published in Cancer Medicine

ISSN: 2045-7634 (Online)
Publisher: Wiley
Country of publisher: United Kingdom
LCC subjects: Medicine: Internal medicine: Neoplasms. Tumors. Oncology. Including cancer and carcinogens
Website: https://onlinelibrary.wiley.com/journal/20457634

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