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A Multiplex Homology-Directed DNA Repair Assay Reveals the Impact of More Than 1,000 BRCA1 Missense Substitution Variants on Protein Function

机译:多重同源定向的DNA修复测定显示超过1,000brca1畸形替代变体对蛋白质功能的影响

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摘要

Loss-of-function pathogenic variants inBRCA1confer a predisposition to breast and ovarian cancer. Genetic testing for sequence changes inBRCA1frequently reveals a missense variant for which the impact on cancer risk and on the molecular function of BRCA1 is unknown. Functional BRCA1 is required for the homology-directed repair (HDR) of double-strand DNA breaks, a critical activity for maintaining genome integrity and tumor suppression. Here, we describe a multiplex HDR reporter assay for concurrently measuring the effects of hundreds of variants of BRCA1 for their role in DNA repair. Using this assay, we characterized the effects of 1,056 amino acid substitutions in the first 192 residues of BRCA1. Benchmarking these results against variants with known effects on DNA repair function or on cancer predisposition, we demonstrate accurate discrimination of loss-of-function versus benign missense variants. We anticipate that this assay can be used to functionally characterize BRCA1 missense variants at scale, even before the variants are observed in results from genetic testing.
机译:功能丧失致病变体inbrca1confer对乳腺癌和卵巢癌的易感性。序列变化的遗传检测inbrca1次数揭示了癌症风险对癌症风险的影响和BRCA1的分子功能未知。双链DNA断裂的同源定向修复(HDR)需要功能性BRCA1,用于维持基因组完整性和肿瘤抑制的关键活性。在这里,我们描述了一种多重HDR报告器测定,用于同时测量BRCA1数百种变体的作用在DNA修复中的作用。使用该测定,我们在BRCA1的前192个残基中表征了1,056个氨基酸取代的作用。这些结果对具有已知对DNA修复功能或癌症倾向的变异性的结果,我们证明了对功能丧失的准确辨别与良性错过变种。我们预期该测定可以用来用来在规模上表征BRCA1畸形变体,甚至在遗传检测结果中观察到变体之前。

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