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OGG1基因编码一种用于修复氧化损伤DNA的酶,并参与人类致癌过程。

The OGG1 gene encodes a repair enzyme for oxidatively damaged DNA and is involved in human carcinogenesis.

作者信息

Shinmura K, Yokota J

机构信息

Biology Division, National Cancer Center Research Institute, Tokyo, Japan.

出版信息

Antioxid Redox Signal. 2001 Aug;3(4):597-609. doi: 10.1089/15230860152542952.

Abstract

8-Hydroxyguanine (oh8G) is a major base lesion produced by reactive oxygen species. oh8G in DNA causes G:C to T:A transversions and, thus, could be responsible for mutations that lead to carcinogenesis. A human DNA glycosylase/AP lyase encoded by the OGG1 gene has an activity to remove directly oh8G from DNA, and suppresses the mutagenic effect of oh8G. OGG1 protein has a helix-hairpin-helix-GPD motif as a domain for both DNA binding and catalysis, a nuclear localization signal, and a mitochondria targeting signal. Among multiple OGG1 isoforms, OGG1-type la is expressed predominantly in human cells and repairs chromosomal DNA in the nucleus. Inactivation of the OGG1 gene in yeast and mice leads to elevated spontaneous mutation frequency in the cells. The human OGG1 gene maps to chromosome 3p26.2, and allelic deletions of this region occur frequently in a variety of human cancers. Moreover, the OGG1 gene is somatically mutated in some cancer cells and is highly polymorphic among human populations. Repair activities of some mutated and polymorphic OGG1 proteins are lower than those of wild-type OGG1-type la-Ser326 protein and, thus, could be involved in human carcinogenesis.

摘要

8-羟基鸟嘌呤(oh8G)是活性氧产生的主要碱基损伤。DNA中的oh8G会导致G:C到T:A的颠换,因此可能是导致致癌的突变的原因。由OGG1基因编码的一种人类DNA糖基化酶/AP裂解酶具有直接从DNA中去除oh8G的活性,并抑制oh8G的诱变作用。OGG1蛋白具有螺旋-发夹-螺旋-GPD基序作为DNA结合和催化的结构域、一个核定位信号和一个线粒体靶向信号。在多种OGG1同工型中,OGG1-type la在人类细胞中主要表达,并修复细胞核中的染色体DNA。酵母和小鼠中OGG1基因的失活导致细胞中自发突变频率升高。人类OGG1基因定位于染色体3p26.2,该区域的等位基因缺失在多种人类癌症中频繁发生。此外,OGG1基因在一些癌细胞中发生体细胞突变,并且在人群中具有高度多态性。一些突变和多态性OGG1蛋白的修复活性低于野生型OGG1-type la-Ser326蛋白,因此可能与人类致癌作用有关。

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