ANO7 African-ancestral genomic diversity and advanced prostate cancer

被引：2

作者：

Jiang, Jue ^{[1
]}

Soh, Pamela X. Y. ^{[1
]}

Mutambirwa, Shingai B. A. ^{[2
]}

Bornman, M. S. Riana ^{[3
]}

Haiman, Christopher A. ^{[4
]}

Hayes, Vanessa M. ^{[1
,3
,5
]}

Jaratlerdsiri, Weerachai ^{[1
]}

机构：

[1] Univ Sydney, Fac Med & Hlth, Charles Perkins Ctr, Sch Med Sci,Ancestry & Hlth Genom Lab, Camperdown, NSW, Australia

[2] Sefako Makgatho Hlth Sci Univ, Dr George Mukhari Acad Hosp, Dept Urol, Medunsa, South Africa

[3] Univ Pretoria, Sch Hlth Syst & Publ Hlth, Pretoria, South Africa

[4] Univ Southern Calif, Ctr Genet Epidemiol, Keck Sch Med, Dept Populat & Publ Hlth Sci, Los Angeles, CA USA

[5] Univ Manchester, Manchester Canc Res Ctr, Manchester, England

来源：

PROSTATE CANCER AND PROSTATIC DISEASES | 2023年 / 27卷 / 3期

基金：

英国医学研究理事会;

关键词：

EXPRESSION; NGEP; LIPRIN-ALPHA-4; INSIGHTS; TARGET; SERVER; G3BP1;

D O I：

10.1038/s41391-023-00722-x

中图分类号：

R73 [肿瘤学];

学科分类号：

100214 ;

摘要：

Background Prostate cancer (PCa) is a significant health burden for African men, with mortality rates more than double global averages. The prostate specific Anoctamin 7 (ANO7) gene linked with poor patient outcomes has recently been identified as the target for an African-specific protein-truncating PCa-risk allele.Methods Here we determined the role of ANO7 in a study of 889 men from southern Africa, leveraging exomic genotyping array PCa case-control data (n = 780, 17 ANO7 alleles) and deep sequenced whole genome data for germline and tumour ANO7 interrogation (n = 109), while providing clinicopathologically matched European-derived sequence data comparative analyses (n = 57). Associated predicted deleterious variants (PDVs) were further assessed for impact using computational protein structure analysis.Results Notably rare in European patients, we found the common African PDV p.Ile740Leu (rs74804606) to be associated with PCa risk in our case-control analysis (Wilcoxon rank-sum test, false discovery rate/FDR = 0.03), while sequencing revealed co-occurrence with the recently reported African-specific deleterious risk variant p.Ser914* (rs60985508). Additional findings included a novel protein-truncating African-specific frameshift variant p.Asp789Leu, African-relevant PDVs associated with altered protein structure at Ca2+ binding sites, early-onset PCa associated with PDVs and germline structural variants in Africans (Linear regression models, -6.42 years, 95% CI = -10.68 to -2.16, P-value = 0.003) and ANO7 as an inter-chromosomal PCa-related gene fusion partner in African derived tumours.Conclusions Here we provide not only validation for ANO7 as an African-relevant protein-altering PCa-risk locus, but additional evidence for a role of inherited and acquired ANO7 variance in the observed phenotypic heterogeneity and African-ancestral health disparity.

引用

页码：558 / 565

页数：8

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