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Patterns and functional implications of rare germline variants across 12 cancer types

机译:跨12种癌症类型的罕见种系变体的模式和功能含义

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摘要

Large-scale cancer sequencing data enable discovery of rare germline cancer susceptibility variants. Here we systematically analyse 4,034 cases from The Cancer Genome Atlas cancer cases representing 12 cancer types. We find that the frequency of rare germline truncations in 114 cancer-susceptibility-associated genes varies widely, from 4% (acute myeloid leukaemia (AML)) to 19% (ovarian cancer), with a notably high frequency of 11% in stomach cancer. Burden testing identifies 13 cancer genes with significant enrichment of rare truncations, some associated with specific cancers (for example, RAD51C, PALB2 and MSH6 in AML, stomach and endometrial cancers, respectively). Significant, tumour-specific loss of heterozygosity occurs in nine genes (ATM, BAP1, BRCA1/2, BRIP1, FANCM, PALB2 and RAD51C/D). Moreover, our homology-directed repair assay of 68 BRCA1 rare missense variants supports the utility of allelic enrichment analysis for characterizing variants of unknown significance. The scale of this analysis and the somatic-germline integration enable the detection of rare variants that may affect individual susceptibility to tumour development, a critical step toward precision medicine.
机译:大规模的癌症测序数据使人们能够发现稀有种系癌症易感性变异。在这里,我们系统地分析了代表12种癌症类型的Cancer Genome Atlas癌症病例中的4,034例。我们发现114种与癌症易感性相关的基因中稀有种系截短的频率差异很大,从4%(急性髓细胞性白血病(AML))到19%(卵巢癌),在胃癌中异常高的频率为11% 。负担测试可鉴定出13种癌基因,这些基因具有罕见截短现象的丰富性,其中一些基因与特定癌症(例如AML,胃癌和子宫内膜癌中的RAD51C,PALB2和MSH6分别相关)。九种基因(ATM,BAP1,BRCA1 / 2,BRIP1,FANCM,PALB2和RAD51C / D)发生了肿瘤特异性的杂合性显着丧失。此外,我们针对68个BRCA1稀有错义变体的同源性定向修复测定支持等位基因富集分析用于表征未知重要性变体的实用性。这种分析的规模和体细胞-种系整合可以检测出可能影响个体对肿瘤发展的敏感性的罕见变体,这是迈向精密医学的关键一步。

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