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Association of Inherited Mutations in DNA Repair Genes with Localized Prostate Cancer

Daniel J. Lee, Ryan Hausler, Anh N. Le, Greg Kelly, Jacquelyn Powers, James Ding, Emily Feld, Heena Desai, Casey Morrison, Abigail Doucette, Peter Gabriel, Renae Judy, JoEllen Weaver, Rachel L. Kember, Scott M. Damrauer, Daniel J. Rader, Susan M. Domchek, Vivek Narayan, Lauren E. Schwartz, Kara N. Maxwell

2021European Urology36 citationsDOIOpen Access PDF

Abstract

BACKGROUND: Identification of germline mutations in DNA repair genes has significant implications for the personalized treatment of individuals with prostate cancer (PrCa). OBJECTIVE: To determine DNA repair genes associated with localized PrCa in a diverse academic biobank and to determine genetic testing burden. DESIGN, SETTING, AND PARTICIPANTS: A cross-sectional study of 2391 localized PrCa patients was carried out. OUTCOME MEASUREMENTS AND STATISTICAL ANALYSIS: Genetic ancestry and mutation rates (excluding somatic interference) in 17 DNA repair genes were determined in 1588 localized PrCa patients and 3273 cancer-free males. Burden testing within individuals of genetically determined European (EUR) and African (AFR) ancestry was performed between biobank PrCa cases and cancer-free biobank and gnomAD males. RESULTS AND LIMITATIONS: AFR individuals with localized PrCa had lower DNA repair gene mutation rates than EUR individuals (1.4% vs 4.0%, p = 0.02). Mutation rates in localized PrCa patients were similar to those in biobank and gnomAD controls (EUR: 4.0% vs 2.8%, p = 0.15, vs 3.1%, p = 0.04; AFR: 1.4% vs 1.8%, p = 0.8, vs 2.1%, p = 0.5). Gene-based rare variant association testing revealed that only BRCA2 mutations were significantly enriched compared with gnomAD controls of EUR ancestry (1.0% vs 0.28%, p = 0.03). Of the participants, 21% and 11% met high-risk and very-high-risk criteria; of them, 3.7% and 6.2% had any germline genetic mutation and 1.0% and 2.5% had a BRCA2 mutation, respectively. Limitations of this study include an analysis of a relatively small, single-institution cohort. CONCLUSIONS: DNA repair gene germline mutation rates are low in an academic biobank cohort of localized PrCa patients, particularly among individuals of AFR genetic ancestry. Mutation rates in genes with published evidence of association with PrCa exceed 2.5% only in high-risk, very-high-risk localized, and node-positive PrCa patients. These findings highlight the importance of risk stratification in localized PrCa patients to identify appropriate patients for germline genetic testing. PATIENT SUMMARY: In the majority of patients who develop localized prostate cancer, germline genetic testing is unlikely to reveal an inherited DNA repair mutation, regardless of race. High-risk features increase the possibility of a germline DNA repair mutation.

Topics & Concepts

MedicineGermline mutationGermlineMutationProstate cancerGeneticsDNA repairGenetic testingCancerGeneInternal medicineOncologyBiologyProstate Cancer Treatment and ResearchProstate Cancer Diagnosis and TreatmentCancer Genomics and Diagnostics
Association of Inherited Mutations in DNA Repair Genes with Localized Prostate Cancer | Litcius