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Universal Patterns of Selection in Cancer and Somatic Tissues

机译:癌症和体细胞组织中的普遍选择模式

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Cancer develops as a result of somatic mutation and clonal selection, but quantitative measures of selection in cancer evolution are lacking. We adapted methods from molecular evolution and applied them to 7,664 tumors across 29 cancer types. Unlike species evolution, positive selection outweighs negative selection during cancer development. On average, 1 coding base substitution/tumor is lost through negative selection, with purifying selection almost absent outside homozygous loss of essential genes. This allows exome-wide enumeration of all driver coding mutations, including outside known cancer genes. On average, tumors carry similar to 4 coding substitutions under positive selection, ranging from 1/tumor in thyroid and testicular cancers to 10/tumor in endometrial and colorectal cancers. Half of driver substitutions occur in yet-to-be-discovered cancer genes. With increasing mutation burden, numbers of driver mutations increase, but not linearly. We systematically catalog cancer genes and show that genes vary extensively in what proportion of mutations are drivers versus passengers.
机译:由于躯体突变和克隆选择,癌症发展,但缺乏癌症演化中的选择性测量。我们改进了分子演化的方法,并将其施加到29种癌症中的7,664种肿瘤。与物种演化不同,阳性选择在癌症发展期间超过了负面选择。平均而言,& 1编码碱替代/肿瘤通过阴性选择丢失,纯化选择几乎不存在外部纯合的必需基因。这允许所有驾驶员编码突变的全面枚举,包括在已知的癌症基因外。平均而言,肿瘤在阳性选择下携带类似于4个编码取代,从甲状腺和睾丸癌中的1 /肿瘤中的& 10 /肿瘤在子宫内膜和结肠直肠癌中。一半的司机取代发生在迄今被发现的癌症基因中。随着突变负担的增加,驾驶员突变数量增加,但不是线性的。我们系统地目录癌症基因并表明基因在突变比例与乘客比例的突变中差异很大。

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