罕见致病结构变异显示出加强非洲男性前列腺癌基因检测的潜力。

Vanessa Hayes, Tingting Gong, Jue Jiang, Riana Bornman, Kazzem Gheybi, Phillip Stricker, Joachim Weischenfeldt, Shingai Mutambirwa
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引用次数: 0

摘要

前列腺癌(PCa)具有高度遗传性,非洲裔男性的风险最大,也最容易致死。基因组数据缺乏代表性意味着种系检测指南排除了非洲男性。虽然结构变异(SV)是导致人类疾病和前列腺肿瘤发生的主要因素,但它们在家族检测和治疗检测中的作用却未得到足够重视。利用临床方法匹配的非洲裔(n = 113)与欧洲裔(n = 57)深度测序 PCa 资源,我们使用最佳拟合致病性预测工作流程询问了 42,966 个高质量种系 SV。我们发现了 15 个潜在致病性 SV,分别代表 12.4% 的非洲患者和 7.0% 的欧洲患者,其中分别有 72% 和 86% 符合种系检测标准建议。值得注意的非洲特异性功能缺失候选基因包括DNA损伤修复基因MLH1和BARD1,以及肿瘤抑制因子FOXP1、WASF1和RB1。这项研究仅代表了散居各地的非洲人中的一小部分,它提出了有关千至百万碱基罕见变异对 PCa 致病性和非洲相关差异的贡献的问题。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Rare pathogenic structural variants show potential to enhance prostate cancer germline testing for African men.

Prostate cancer (PCa) is highly heritable, with men of African ancestry at greatest risk and associated lethality. Lack of representation in genomic data means germline testing guidelines exclude for African men. Established that structural variations (SVs) are major contributors to human disease and prostate tumourigenesis, their role is under-appreciated in familial and therapeutic testing. Utilising a clinico-methodologically matched African (n = 113) versus European (n = 57) deep-sequenced PCa resource, we interrogated 42,966 high-quality germline SVs using a best-fit pathogenicity prediction workflow. We identified 15 potentially pathogenic SVs representing 12.4% African and 7.0% European patients, of which 72% and 86% met germline testing standard-of-care recommendations, respectively. Notable African-specific loss-of-function gene candidates include DNA damage repair MLH1 and BARD1 and tumour suppressors FOXP1, WASF1 and RB1. Representing only a fraction of the vast African diaspora, this study raises considerations with respect to the contribution of kilo-to-mega-base rare variants to PCa pathogenicity and African associated disparity.

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