Association of rare, recurrent nonsynonymous variants in the germline of prostate cancer patients of African ancestry

Jun Wei; Jennifer Beebe-Dimmer; Zhuqing Shi; Christopher Sample; Guifang Yan; Andrew S. Rifkin; Azita Sadeghpour; Marta Gielzak; Sodam Choi; David Moon; S. Lilly Zheng; Brian T. Helfand; Patrick C. Walsh; Jianfeng Xu; Kathleen A. Cooney; William B. Isaacs

doi:10.1002/pros.24477

Association of rare, recurrent nonsynonymous variants in the germline of prostate cancer patients of African ancestry

Jun Wei, Jennifer Beebe-Dimmer, Zhuqing Shi, Christopher Sample, Guifang Yan, Andrew S. Rifkin, Azita Sadeghpour, Marta Gielzak, Sodam Choi, David Moon, S. Lilly Zheng, Brian T. Helfand, Patrick C. Walsh, Jianfeng Xu, Kathleen A. Cooney, William B. Isaacs

Research output: Contribution to journal › Article › peer-review

Abstract

Background: Although men of African ancestry (AA) have the highest mortality rate from prostate cancer (PCa), relatively little is known about the germline variants that are associated with PCa risk in AA men. The goal of this study is to systematically evaluate rare, recurrent nonsynonymous variants across the exome for their association with PCa in AA men. Methods: Whole exome sequencing (WES) of germline DNA in two AA PCa patient cohorts of Johns Hopkins Hospital (N = 960) and Wayne State University (N = 747) was performed. All nonsynonymous variants present in both case cohorts, with a carrier rate between 0.5% and 1%, were identified. Their carrier rates were compared with rates from 8128 African/African American (AFR) control subjects from The Genome Aggregation Database (gnomAD) using Fisher's exact test. Significant variants, defined as false discovery rate (FDR) adjusted p-value ≤ 0.05, were further evaluated in AA PCa cases (N = 132) and controls (N = 1184) from the UK Biobank (UKB). Results: Two variants reached a pre-specified statistical significance level. The first was p.R14Q in GPRC5C (found in 0.47% of PCa cases and 0.01% of population controls); odds ratio (OR) for PCa was 37.46 (95% confidence interval CI 4.68–299.72), p_exact = 7.01E-06, FDR-adjusted p-value = 0.05. The second was p.R511Q in IGF1R (found in 0.53% of PCa cases and 0.01% of population controls); OR for PCa was 21.54 (95%CI 4.65–99.76), p_exact = 5.51E-06, FDR-adjusted p-value = 0.05. The mean percentage of African ancestry was similar between variant carriers and noncarriers of each variant, p > 0.05. In the UKB AA men, GPRC5C R14Q was 0.76% and 0.08% in cases and controls, respectively, OR for PCa was 9.00 (95%CI 0.56–145.23), p_exact = 0.19. However, IGF1R R511Q was not found in cases or controls. Conclusions: This WES study identified two rare, recurrent nonsynonymous PCa risk-associated variants in AA. Confirmation in additional large populations of AA PCa cases and controls is required.

Original language	English (US)
Pages (from-to)	454-461
Number of pages	8
Journal	Prostate
Volume	83
Issue number	5
DOIs	https://doi.org/10.1002/pros.24477
State	Published - Apr 2023

Keywords

African ancestry (AA)
germline
nonsynonymous mutation
prostate cancer
whole exome sequencing (WES)

ASJC Scopus subject areas

Urology
Oncology

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10.1002/pros.24477

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Wei, J., Beebe-Dimmer, J., Shi, Z., Sample, C., Yan, G., Rifkin, A. S., Sadeghpour, A., Gielzak, M., Choi, S., Moon, D., Zheng, S. L., Helfand, B. T., Walsh, P. C., Xu, J., Cooney, K. A., & Isaacs, W. B. (2023). Association of rare, recurrent nonsynonymous variants in the germline of prostate cancer patients of African ancestry. Prostate, 83(5), 454-461. https://doi.org/10.1002/pros.24477

Wei, J, Beebe-Dimmer, J, Shi, Z, Sample, C, Yan, G, Rifkin, AS, Sadeghpour, A, Gielzak, M, Choi, S, Moon, D, Zheng, SL, Helfand, BT, Walsh, PC, Xu, J, Cooney, KA & Isaacs, WB 2023, 'Association of rare, recurrent nonsynonymous variants in the germline of prostate cancer patients of African ancestry', Prostate, vol. 83, no. 5, pp. 454-461. https://doi.org/10.1002/pros.24477

@article{86efb5081d8f457fb9847e20746c5855,

title = "Association of rare, recurrent nonsynonymous variants in the germline of prostate cancer patients of African ancestry",

abstract = "Background: Although men of African ancestry (AA) have the highest mortality rate from prostate cancer (PCa), relatively little is known about the germline variants that are associated with PCa risk in AA men. The goal of this study is to systematically evaluate rare, recurrent nonsynonymous variants across the exome for their association with PCa in AA men. Methods: Whole exome sequencing (WES) of germline DNA in two AA PCa patient cohorts of Johns Hopkins Hospital (N = 960) and Wayne State University (N = 747) was performed. All nonsynonymous variants present in both case cohorts, with a carrier rate between 0.5% and 1%, were identified. Their carrier rates were compared with rates from 8128 African/African American (AFR) control subjects from The Genome Aggregation Database (gnomAD) using Fisher's exact test. Significant variants, defined as false discovery rate (FDR) adjusted p-value ≤ 0.05, were further evaluated in AA PCa cases (N = 132) and controls (N = 1184) from the UK Biobank (UKB). Results: Two variants reached a pre-specified statistical significance level. The first was p.R14Q in GPRC5C (found in 0.47% of PCa cases and 0.01% of population controls); odds ratio (OR) for PCa was 37.46 (95% confidence interval CI 4.68–299.72), pexact = 7.01E-06, FDR-adjusted p-value = 0.05. The second was p.R511Q in IGF1R (found in 0.53% of PCa cases and 0.01% of population controls); OR for PCa was 21.54 (95%CI 4.65–99.76), pexact = 5.51E-06, FDR-adjusted p-value = 0.05. The mean percentage of African ancestry was similar between variant carriers and noncarriers of each variant, p > 0.05. In the UKB AA men, GPRC5C R14Q was 0.76% and 0.08% in cases and controls, respectively, OR for PCa was 9.00 (95%CI 0.56–145.23), pexact = 0.19. However, IGF1R R511Q was not found in cases or controls. Conclusions: This WES study identified two rare, recurrent nonsynonymous PCa risk-associated variants in AA. Confirmation in additional large populations of AA PCa cases and controls is required.",

keywords = "African ancestry (AA), germline, nonsynonymous mutation, prostate cancer, whole exome sequencing (WES)",

author = "Jun Wei and Jennifer Beebe-Dimmer and Zhuqing Shi and Christopher Sample and Guifang Yan and Rifkin, {Andrew S.} and Azita Sadeghpour and Marta Gielzak and Sodam Choi and David Moon and Zheng, {S. Lilly} and Helfand, {Brian T.} and Walsh, {Patrick C.} and Jianfeng Xu and Cooney, {Kathleen A.} and Isaacs, {William B.}",

note = "Publisher Copyright: {\textcopyright} 2022 Wiley Periodicals LLC.",

year = "2023",

month = apr,

doi = "10.1002/pros.24477",

language = "English (US)",

volume = "83",

pages = "454--461",

journal = "Prostate",

issn = "0270-4137",

publisher = "Wiley-Liss Inc.",

number = "5",

}

TY - JOUR

T1 - Association of rare, recurrent nonsynonymous variants in the germline of prostate cancer patients of African ancestry

AU - Wei, Jun

AU - Beebe-Dimmer, Jennifer

AU - Shi, Zhuqing

AU - Sample, Christopher

AU - Yan, Guifang

AU - Rifkin, Andrew S.

AU - Sadeghpour, Azita

AU - Gielzak, Marta

AU - Choi, Sodam

AU - Moon, David

AU - Zheng, S. Lilly

AU - Helfand, Brian T.

AU - Walsh, Patrick C.

AU - Xu, Jianfeng

AU - Cooney, Kathleen A.

AU - Isaacs, William B.

PY - 2023/4

Y1 - 2023/4

N2 - Background: Although men of African ancestry (AA) have the highest mortality rate from prostate cancer (PCa), relatively little is known about the germline variants that are associated with PCa risk in AA men. The goal of this study is to systematically evaluate rare, recurrent nonsynonymous variants across the exome for their association with PCa in AA men. Methods: Whole exome sequencing (WES) of germline DNA in two AA PCa patient cohorts of Johns Hopkins Hospital (N = 960) and Wayne State University (N = 747) was performed. All nonsynonymous variants present in both case cohorts, with a carrier rate between 0.5% and 1%, were identified. Their carrier rates were compared with rates from 8128 African/African American (AFR) control subjects from The Genome Aggregation Database (gnomAD) using Fisher's exact test. Significant variants, defined as false discovery rate (FDR) adjusted p-value ≤ 0.05, were further evaluated in AA PCa cases (N = 132) and controls (N = 1184) from the UK Biobank (UKB). Results: Two variants reached a pre-specified statistical significance level. The first was p.R14Q in GPRC5C (found in 0.47% of PCa cases and 0.01% of population controls); odds ratio (OR) for PCa was 37.46 (95% confidence interval CI 4.68–299.72), pexact = 7.01E-06, FDR-adjusted p-value = 0.05. The second was p.R511Q in IGF1R (found in 0.53% of PCa cases and 0.01% of population controls); OR for PCa was 21.54 (95%CI 4.65–99.76), pexact = 5.51E-06, FDR-adjusted p-value = 0.05. The mean percentage of African ancestry was similar between variant carriers and noncarriers of each variant, p > 0.05. In the UKB AA men, GPRC5C R14Q was 0.76% and 0.08% in cases and controls, respectively, OR for PCa was 9.00 (95%CI 0.56–145.23), pexact = 0.19. However, IGF1R R511Q was not found in cases or controls. Conclusions: This WES study identified two rare, recurrent nonsynonymous PCa risk-associated variants in AA. Confirmation in additional large populations of AA PCa cases and controls is required.

AB - Background: Although men of African ancestry (AA) have the highest mortality rate from prostate cancer (PCa), relatively little is known about the germline variants that are associated with PCa risk in AA men. The goal of this study is to systematically evaluate rare, recurrent nonsynonymous variants across the exome for their association with PCa in AA men. Methods: Whole exome sequencing (WES) of germline DNA in two AA PCa patient cohorts of Johns Hopkins Hospital (N = 960) and Wayne State University (N = 747) was performed. All nonsynonymous variants present in both case cohorts, with a carrier rate between 0.5% and 1%, were identified. Their carrier rates were compared with rates from 8128 African/African American (AFR) control subjects from The Genome Aggregation Database (gnomAD) using Fisher's exact test. Significant variants, defined as false discovery rate (FDR) adjusted p-value ≤ 0.05, were further evaluated in AA PCa cases (N = 132) and controls (N = 1184) from the UK Biobank (UKB). Results: Two variants reached a pre-specified statistical significance level. The first was p.R14Q in GPRC5C (found in 0.47% of PCa cases and 0.01% of population controls); odds ratio (OR) for PCa was 37.46 (95% confidence interval CI 4.68–299.72), pexact = 7.01E-06, FDR-adjusted p-value = 0.05. The second was p.R511Q in IGF1R (found in 0.53% of PCa cases and 0.01% of population controls); OR for PCa was 21.54 (95%CI 4.65–99.76), pexact = 5.51E-06, FDR-adjusted p-value = 0.05. The mean percentage of African ancestry was similar between variant carriers and noncarriers of each variant, p > 0.05. In the UKB AA men, GPRC5C R14Q was 0.76% and 0.08% in cases and controls, respectively, OR for PCa was 9.00 (95%CI 0.56–145.23), pexact = 0.19. However, IGF1R R511Q was not found in cases or controls. Conclusions: This WES study identified two rare, recurrent nonsynonymous PCa risk-associated variants in AA. Confirmation in additional large populations of AA PCa cases and controls is required.

KW - African ancestry (AA)

KW - germline

KW - nonsynonymous mutation

KW - prostate cancer

KW - whole exome sequencing (WES)

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UR - http://www.scopus.com/inward/citedby.url?scp=85145205627&partnerID=8YFLogxK

U2 - 10.1002/pros.24477

DO - 10.1002/pros.24477

M3 - Article

C2 - 36567534

AN - SCOPUS:85145205627

SN - 0270-4137

VL - 83

SP - 454

EP - 461

JO - Prostate

JF - Prostate

IS - 5

ER -

Association of rare, recurrent nonsynonymous variants in the germline of prostate cancer patients of African ancestry

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