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Mutational spectra of human cancer.

机译:人类癌症的突变谱。

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The purpose of this review is to summarize the evidence that can be used to reconstruct the etiology of human cancers from mutations found in tumors. Mutational spectra of the tumor suppressor gene p53 (TP53) are tumor specific. In several cases, these mutational spectra can be linked to exogenous carcinogens, most notably for sunlight-associated skin cancers, tobacco-associated lung cancers, and aristolochic acid-related urothelial tumors. In the TP53 gene, methylated CpG dinucleotides are sequences selectively targeted by endogenous and exogenous mutagenic processes. Recent high-throughput sequencing efforts analyzing a large number of genes in cancer genomes have so far, for the most part, produced mutational spectra similar to those in TP53 but have unveiled a previously unrecognized common G to C transversion mutation signature at GpA dinucleotides in breast cancers and several other cancers. Unraveling the origin of these G to C mutations will be of importance for understanding cancer etiology.
机译:这篇综述的目的是总结可用于从肿瘤中发现的突变来重建人类癌症病因的证据。抑癌基因p53(TP53)的突变谱是肿瘤特异性的。在某些情况下,这些突变谱可以与外源致癌物相关,最明显的是与阳光有关的皮肤癌,与烟草有关的肺癌和与马兜铃酸有关的尿路上皮肿瘤。在TP53基因中,甲基化的CpG二核苷酸是内源性和外源性诱变过程选择性靶向的序列。迄今为止,最近进行的高通量测序工作已分析了癌症基因组中的大量基因,在很大程度上已产生了与TP53相似的突变谱,但在乳腺GpA二核苷酸上揭示了以前无法识别的常见G到C转换突变签名癌症和其他几种癌症。阐明这些G到C突变的起源对于理解癌症病因至关重要。

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