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首页> 外文期刊>Acta biochimica Polonica >Bacterial DNA repair genes and their eukaryotic homologues: 2. Role of bacterial mutator gene homologues in human disease. Overview of nucleotide pool sanitization and mismatch repair systems
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Bacterial DNA repair genes and their eukaryotic homologues: 2. Role of bacterial mutator gene homologues in human disease. Overview of nucleotide pool sanitization and mismatch repair systems

机译:细菌DNA修复基因及其真核同源物:2.细菌突变基因同源物在人类疾病中的作用。核苷酸池消毒和错配修复系统概述

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Since the discovery of the first E. coli mutator gene, mutT, most of the mutations inducing elevated spontaneous mutation rates could be clearly attributed to defects in DNA repair. MutT turned out to be a pyrophosphohydrolase hydrolyzing 8-oxodGTP, thus preventing its incorporation into DNA and suppresing the occurrence of spontaneous AT→CG transversions. Most of the bacterial mutator genes appeared to be evolutionarily conserved, and scientists were continuously searching for contribution of DNA repair deficiency in human diseases, especially carcinogenesis. Yet a human MutT homologue - hMTH1 protein - was found to be overexpressed rather than inactivated in many human diseases, including cancer. The interest in DNA repair contribution to human diseases exploded with the observation that germline mutations in mismatch repair (MMR) genes predispose to hereditary non-polyposis colorectal cancer (HNPCC). Despite our continuously growing knowledge about DNA repair we still do not fully understand how the mutator phenotype contributes to specific forms of human diseases.
机译:自从发现第一个大肠杆菌突变基因mutT以来,大多数诱发自发突变率升高的突变都可以明确归因于DNA修复的缺陷。 MutT证明是一种水解8-oxodGTP的焦磷酸水解酶,因此可防止将其掺入DNA并阻止自发发生AT→CG转化。大多数细菌突变基因似乎在进化上是保守的,科学家们一直在寻找DNA修复缺陷在人类疾病中的作用,特别是在癌变中。然而,人类MutT同源物-hMTH1蛋白-在许多人类疾病(包括癌症)中被过度表达而不是失活。 DNA修复对人类疾病的贡献引起了人们的关注,因为观察到错配修复(MMR)基因的种系突变易患遗传性非息肉性结直肠癌(HNPCC)。尽管我们对DNA修复的知识不断增长,但我们仍不完全了解突变体表型如何导致特定形式的人类疾病。

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