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Pathogenic germline DNA repair gene and HOXB13 mutations in men with metastatic prostate cancer

Publication ,  Journal Article
Boyle, JL; Hahn, AW; Kapron, AL; Kohlmann, W; Greenberg, SE; Parnell, TJ; Teerlink, CC; Maughan, BL; Feng, BJ; Cannon-Albright, L; Agarwal, N ...
Published in: JCO Precision Oncology
January 1, 2019

PURPOSE Germline mutations in DNA repair (DR) genes and susceptibility genes CDKN2A and HOXB13 have previously been associated with prostate cancer (PC) incidence and/or progression. However, the role and prevalence of this class of mutations in metastatic PC (mPC) are not fully understood. PATIENTS AND METHODS To evaluate the frequency of pathogenic/likely pathogenic germline variants (PVs/ LPVs) in men with mPC, this study sequenced 38 DR genes, CDKN2A, and HOXB13 in a predominantly white cohort of 317 patients with mPC. A PC registry at the University of Utah was used for patient sample acquisition and retrospective clinical data collection. Deep target sequencing allowed for germline and copy number variant analyses. Validated PVs/LPVs were integrated with clinical and demographic data for statistical correlation analyses. RESULTS All pathogenic variants were found in men self-reported as white, with a carrier frequency of 8.5% (DR genes, 7.3%; CDKN2A/HOXB13, 1.2%). Consistent with previous reports, mutations were most frequently identified in the breast cancer susceptibility gene BRCA2. It was also found that 50% of identified PVs/LPVs were categorized as founder mutations with European origins. Correlation analyses did not support a trend toward more advanced or earlier-onset disease in comparisons between carriers and noncarriers of deleterious DR or HOXB13 G84E mutations. CONCLUSION These findings demonstrate a lower prevalence of germline PVs/LPVs in an unselected, predominantly white mPC cohort than previously reported, which may have implications for the design of clinical trials testing targeted therapies. Larger studies in broad and diverse populations are needed to more accurately define the prevalence of germline mutations in men with mPC.

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Published In

JCO Precision Oncology

DOI

EISSN

2473-4284

Publication Date

January 1, 2019

Volume

3

Start / End Page

139 / 151

Related Subject Headings

  • 3211 Oncology and carcinogenesis
 

Citation

APA
Chicago
ICMJE
MLA
NLM
Boyle, J. L., Hahn, A. W., Kapron, A. L., Kohlmann, W., Greenberg, S. E., Parnell, T. J., … Cooney, K. A. (2019). Pathogenic germline DNA repair gene and HOXB13 mutations in men with metastatic prostate cancer. JCO Precision Oncology, 3, 139–151. https://doi.org/10.1200/PO.19.00284
Boyle, J. L., A. W. Hahn, A. L. Kapron, W. Kohlmann, S. E. Greenberg, T. J. Parnell, C. C. Teerlink, et al. “Pathogenic germline DNA repair gene and HOXB13 mutations in men with metastatic prostate cancer.” JCO Precision Oncology 3 (January 1, 2019): 139–51. https://doi.org/10.1200/PO.19.00284.
Boyle JL, Hahn AW, Kapron AL, Kohlmann W, Greenberg SE, Parnell TJ, et al. Pathogenic germline DNA repair gene and HOXB13 mutations in men with metastatic prostate cancer. JCO Precision Oncology. 2019 Jan 1;3:139–51.
Boyle, J. L., et al. “Pathogenic germline DNA repair gene and HOXB13 mutations in men with metastatic prostate cancer.” JCO Precision Oncology, vol. 3, Jan. 2019, pp. 139–51. Scopus, doi:10.1200/PO.19.00284.
Boyle JL, Hahn AW, Kapron AL, Kohlmann W, Greenberg SE, Parnell TJ, Teerlink CC, Maughan BL, Feng BJ, Cannon-Albright L, Agarwal N, Cooney KA. Pathogenic germline DNA repair gene and HOXB13 mutations in men with metastatic prostate cancer. JCO Precision Oncology. 2019 Jan 1;3:139–151.

Published In

JCO Precision Oncology

DOI

EISSN

2473-4284

Publication Date

January 1, 2019

Volume

3

Start / End Page

139 / 151

Related Subject Headings

  • 3211 Oncology and carcinogenesis