Inherited DNA-Repair Gene Mutations in Men with Metastatic Prostate Cancer

Colin C. Pritchard; Joaquı́n Mateo; Michael F. Walsh; Navonil De Sarkar; Wassim Abida; Himisha Beltran; Andrea Garofalo; Roman Gulati; Suzanne Carreira; Rosalind A. Eeles; Olivier Elemento; Mark A. Rubin; Dan R. Robinson; Robert J. Lonigro; Maha Hussain; Arul M. Chinnaiyan; Jake Vinson; Julie Filipenko; Levi A. Garraway; Mary‐Ellen Taplin; Saud H. AlDubayan; G. Celine Han; Mallory Beightol; Colm Morrissey; Belinda Nghiem; Heather H. Cheng; Bruce Montgomery; Tom Walsh; Silvia Casadei; Michael F. Berger; Liying Zhang; Ahmet Zehir; Joseph Vijai; Howard I. Scher; Charles L. Sawyers; Nikolaus Schultz; Philip W. Kantoff; David B. Solit; Mark E. Robson; Eliezer M. Van Allen; Kenneth Offit; Johann S. de Bono; Peter S. Nelson

doi:10.1056/nejmoa1603144

Inherited DNA-Repair Gene Mutations in Men with Metastatic Prostate Cancer

Colin C. Pritchard(University of Washington), Joaquı́n Mateo(Royal Marsden Hospital), Michael F. Walsh(Memorial Sloan Kettering Cancer Center), Navonil De Sarkar(Memorial Sloan Kettering Cancer Center), Wassim Abida(Memorial Sloan Kettering Cancer Center), Himisha Beltran(Cornell University), Andrea Garofalo(Dana-Farber Cancer Institute), Roman Gulati(Fred Hutch Cancer Center), Suzanne Carreira(Royal Marsden Hospital), Rosalind A. Eeles(Royal Marsden Hospital), Olivier Elemento(Cornell University), Mark A. Rubin(Cornell University), Dan R. Robinson(University of Michigan–Ann Arbor), Robert J. Lonigro(University of Michigan–Ann Arbor), Maha Hussain(University of Michigan–Ann Arbor), Arul M. Chinnaiyan(University of Michigan–Ann Arbor), Jake Vinson, Julie Filipenko, Levi A. Garraway(Dana-Farber Cancer Institute), Mary‐Ellen Taplin(Dana-Farber Cancer Institute), Saud H. AlDubayan(Dana-Farber Cancer Institute), G. Celine Han(Dana-Farber Cancer Institute), Mallory Beightol(University of Washington), Colm Morrissey(University of Washington), Belinda Nghiem(University of Washington), Heather H. Cheng(University of Washington), Bruce Montgomery(University of Washington), Tom Walsh(University of Washington), Silvia Casadei(University of Washington), Michael F. Berger(Memorial Sloan Kettering Cancer Center), Liying Zhang(Memorial Sloan Kettering Cancer Center), Ahmet Zehir(Memorial Sloan Kettering Cancer Center), Joseph Vijai(Memorial Sloan Kettering Cancer Center), Howard I. Scher(Memorial Sloan Kettering Cancer Center), Charles L. Sawyers(Howard Hughes Medical Institute), Nikolaus Schultz(Memorial Sloan Kettering Cancer Center), Philip W. Kantoff(Memorial Sloan Kettering Cancer Center), David B. Solit(Memorial Sloan Kettering Cancer Center), Mark E. Robson(Memorial Sloan Kettering Cancer Center), Eliezer M. Van Allen(Dana-Farber Cancer Institute), Kenneth Offit(Memorial Sloan Kettering Cancer Center), Johann S. de Bono(Royal Marsden Hospital), Peter S. Nelson(Fred Hutch Cancer Center)

New England Journal of Medicine

July 6, 2016

10.1056/nejmoa1603144

Cited by 1,654Open Access

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Abstract

BACKGROUND: Inherited mutations in DNA-repair genes such as BRCA2 are associated with increased risks of lethal prostate cancer. Although the prevalence of germline mutations in DNA-repair genes among men with localized prostate cancer who are unselected for family predisposition is insufficient to warrant routine testing, the frequency of such mutations in patients with metastatic prostate cancer has not been established. METHODS: We recruited 692 men with documented metastatic prostate cancer who were unselected for family history of cancer or age at diagnosis. We isolated germline DNA and used multiplex sequencing assays to assess mutations in 20 DNA-repair genes associated with autosomal dominant cancer-predisposition syndromes. RESULTS: A total of 84 germline DNA-repair gene mutations that were presumed to be deleterious were identified in 82 men (11.8%); mutations were found in 16 genes, including BRCA2 (37 men [5.3%]), ATM (11 [1.6%]), CHEK2 (10 [1.9% of 534 men with data]), BRCA1 (6 [0.9%]), RAD51D (3 [0.4%]), and PALB2 (3 [0.4%]). Mutation frequencies did not differ according to whether a family history of prostate cancer was present or according to age at diagnosis. Overall, the frequency of germline mutations in DNA-repair genes among men with metastatic prostate cancer significantly exceeded the prevalence of 4.6% among 499 men with localized prostate cancer (P<0.001), including men with high-risk disease, and the prevalence of 2.7% in the Exome Aggregation Consortium, which includes 53,105 persons without a known cancer diagnosis (P<0.001). CONCLUSIONS: In our multicenter study, the incidence of germline mutations in genes mediating DNA-repair processes among men with metastatic prostate cancer was 11.8%, which was significantly higher than the incidence among men with localized prostate cancer. The frequencies of germline mutations in DNA-repair genes among men with metastatic disease did not differ significantly according to age at diagnosis or family history of prostate cancer. (Funded by Stand Up To Cancer and others.).

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