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DNA碱基切除修复作为分子流行病学研究中的生物标志物

DNA base excision repair as a biomarker in molecular epidemiology studies.

作者信息

Collins Andrew R, Gaivão Isabel

机构信息

Department of Nutrition, Faculty of Medicine, University of Oslo, 0316 Oslo, Norway.

出版信息

Mol Aspects Med. 2007 Jun-Aug;28(3-4):307-22. doi: 10.1016/j.mam.2007.05.005. Epub 2007 Jun 2.

Abstract

Base excision repair can be measured in human lymphocytes by a variety of techniques, the most convenient of which are probably in vitro assays of the activity of a cell extract on a DNA substrate containing specific lesions such as 8-oxoguanine. Inter-individual variation in base excision repair ranges from about 3-fold to 10-fold in different studies. Repair has been variously reported to decline or to increase with the age of the individual. Few studies of environmental or occupational exposure and repair have been carried out, but it seems that styrene exposure induces base excision repair activity. In several nutritional intervention trials, with kiwifruit, coenzyme Q(10) and carrots, a significant enhancement of repair has been noted. Activity of 8-oxoguanine DNA glycosylase is significantly affected by the Ser326Cys polymorphism in hOGG1. In cancer case-control studies, low repair activity is consistently associated with occurrence of the disease.

摘要

碱基切除修复可通过多种技术在人类淋巴细胞中进行检测,其中最便捷的可能是对含有特定损伤(如8-氧代鸟嘌呤)的DNA底物进行细胞提取物活性的体外检测。在不同研究中,个体间碱基切除修复的差异范围约为3倍至10倍。关于修复随个体年龄增长是下降还是增加,已有不同的报道。关于环境或职业暴露与修复的研究很少,但似乎苯乙烯暴露会诱导碱基切除修复活性。在几项使用猕猴桃、辅酶Q(10)和胡萝卜的营养干预试验中,已注意到修复有显著增强。hOGG1基因中的Ser326Cys多态性会显著影响8-氧代鸟嘌呤DNA糖基化酶的活性。在癌症病例对照研究中,低修复活性始终与疾病的发生相关。

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