Targeted sequencing for hereditary breast and ovarian cancer in BRCA1/2-negative families reveals complex genetic architecture and phenocopies.

IF 3.3 Q2 GENETICS & HEREDITY
HGG Advances Pub Date : 2024-07-18 Epub Date: 2024-05-10 DOI:10.1016/j.xhgg.2024.100306
Jocelyn N Plowman, Evanjalina J Matoy, Lavanya V Uppala, Samantha B Draves, Cynthia J Watson, Bridget A Sefranek, Mark L Stacey, Samuel P Anderson, Michael A Belshan, Elizabeth E Blue, Chad D Huff, Yusi Fu, Holly A F Stessman
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引用次数: 0

Abstract

Approximately 20% of breast cancer cases are attributed to increased family risk, yet variation in BRCA1/2 can only explain 20%-25% of cases. Historically, only single gene or single variant testing were common in at-risk family members, and further sequencing studies were rarely offered after negative results. In this study, we applied an efficient and inexpensive targeted sequencing approach to provide molecular diagnoses in 245 human samples representing 134 BRCA mutation-negative (BRCAX) hereditary breast and ovarian cancer (HBOC) families recruited from 1973 to 2019 by Dr. Henry Lynch. Sequencing identified 391 variants, which were functionally annotated and ranked based on their predicted clinical impact. Known pathogenic CHEK2 breast cancer variants were identified in five BRCAX families in this study. While BRCAX was an inclusion criterion for this study, we still identified a pathogenic BRCA2 variant (p.Met192ValfsTer13) in one family. A portion of BRCAX families could be explained by other hereditary cancer syndromes that increase HBOC risk: Li-Fraumeni syndrome (gene: TP53) and Lynch syndrome (gene: MSH6). Interestingly, many families carried additional variants of undetermined significance (VOUSs) that may further modify phenotypes of syndromic family members. Ten families carried more than one potential VOUS, suggesting the presence of complex multi-variant families. Overall, nine BRCAX HBOC families in our study may be explained by known likely pathogenic/pathogenic variants, and six families carried potential VOUSs, which require further functional testing. To address this, we developed a functional assay where we successfully re-classified one family's PMS2 VOUS as benign.

林奇纪念生物库中 BRCA1/2 阴性家族遗传性乳腺癌和卵巢癌的定向测序揭示了复杂的遗传结构和表型。
约 20% 的乳腺癌病例是由于家族风险增加所致;但 BRCA1/2 变异只能解释 20-25% 的病例。一直以来,只有单基因或单个变异检测在高危家族成员中比较常见,而且在检测结果呈阴性后也很少提供进一步的测序研究。在这项研究中,我们采用了一种高效、廉价的靶向测序方法,对亨利-林奇博士(Dr. Henry Lynch)在 1973-2019 年间招募的 134 个 BRCA 突变阴性(BRCAX)遗传性乳腺癌和卵巢癌(HBOC)家族的 245 份人类样本进行了分子诊断。测序确定了 391 个变异,并根据其预测的临床影响对这些变异进行了功能注释和排序。本研究在五个 BRCAX 家系中发现了已知的 CHEK2 乳腺癌致病变异。虽然 BRCAX 是本研究的一个纳入标准,但我们仍在一个家族中发现了致病性 BRCA2 变异(p.Met192ValfsTer13)。部分 BRCAX 家系可由其他增加 HBOC 风险的遗传性癌症综合征解释:Li-Fraumeni 综合征(基因:TP53)和林奇综合征(基因:MSH6)。有趣的是,许多家族还携带了其他意义未定的变异(VOUS),这些变异可能会进一步改变综合征家族成员的表型。有 10 个家族携带一个以上的潜在 VOUS,这表明存在复杂的多变异家族。总的来说,在我们的研究中,有 9 个 BRCAX HBOC 家系可以用已知的可能致病/致病变异来解释,有 6 个家系带有潜在的 VOUSs,这需要进一步的功能测试。为了解决这个问题,我们开发了一种功能检测方法,成功地将一个家族的 PMS2 VOUS 重新归类为良性。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
HGG Advances
HGG Advances Biochemistry, Genetics and Molecular Biology-Molecular Medicine
CiteScore
4.30
自引率
4.50%
发文量
69
审稿时长
14 weeks
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