[Repair of oxidized guanine in mammals: OGG1 genes].

J P Radicella, S Boiteux
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Abstract

This paper reviews the present state of the studies on the repair of a major oxydative lesion on DNA, the 8-oxo-guanine (8-OxoG). This modified base has been proved to be highly mutagenic and therefore implicated in the ethiology of several pathologies. The cloning of the yeast OGG1 gene, a functional homolog of the fpg from bacteria, allowed the isolation of the mammalian homologs. These genes code for 8-OxoG DNA glycosylases/lyases, whose biochemical properties are consistent with their postulated role as the main defence against the genetic instability induced by the presence of 8-OxoG in DNA. This, together with the mutator phenotype of the yeast ogg1 mutant strains, make of the human OGG1 a candidate for a cancer predisposition gene. The localization of this gene to chromosome 3p and other evidences discussed in this paper indicate that OGG1 could be a tumor suppressor gene implicated in lung cancer.

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[哺乳动物氧化鸟嘌呤修复:OGG1基因]。
本文综述了DNA主要氧化损伤8-氧鸟嘌呤(8-OxoG)修复的研究现状。这种修饰的碱基已被证明是高度诱变的,因此与几种病理的伦理学有关。酵母OGG1基因的克隆,与细菌中fpg的功能同源,允许分离哺乳动物同源物。这些基因编码8-OxoG DNA糖基酶/裂解酶,其生化特性与它们作为防止DNA中8-OxoG存在引起的遗传不稳定性的主要防御作用相一致。这与酵母ogg1突变株的突变表型一起,使人类ogg1成为癌症易感性基因的候选基因。该基因在染色体3p上的定位以及本文讨论的其他证据表明,OGG1可能是一个与肺癌有关的肿瘤抑制基因。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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