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DNA中的单链断裂而非氧化性DNA碱基损伤会阻断HeLa细胞核提取物中RNA聚合酶II的转录延伸。

Single-stranded breaks in DNA but not oxidative DNA base damages block transcriptional elongation by RNA polymerase II in HeLa cell nuclear extracts.

作者信息

Kathe Scott D, Shen Guang-Ping, Wallace Susan S

机构信息

Department of Microbiology and Molecular Genetics, The Markey Center for Molecular Genetics, University of Vermont, Burlington, Vermont 05405-0068, USA.

出版信息

J Biol Chem. 2004 Apr 30;279(18):18511-20. doi: 10.1074/jbc.M313598200. Epub 2004 Feb 21.

Abstract

Transcription and repair of many DNA helix-distorting lesions such as cyclobutane pyrimidine dimers have been shown to be coupled in cells across phyla from bacteria to humans. The signal for transcription-coupled repair appears to be a stalled transcription complex at the lesion site. To determine whether oxidative DNA lesions can block correctly initiated human RNA polymerase II, we examined the effect of site-specifically introduced oxidative damages on transcription in HeLa cell nuclear extracts. We found that transcription was blocked by single-stranded breaks, common oxidative DNA lesions, when present in the transcribed strand of the transcription template. Cyclobutane pyrimidine dimers, which have been previously shown to block transcription both in vitro and in vivo, also blocked transcription in the HeLa cell nuclear transcription assay. In contrast, the oxidative DNA base lesions, 8-oxoguanine, 5-hydroxycytosine, and thymine glycol did not inhibit transcription, although pausing was observed with the thymine glycol lesion. Thus, DNA strand breaks but not oxidative DNA base damages blocked transcription by RNA polymerase II.

摘要

从细菌到人类的各生物门中,许多扭曲DNA螺旋的损伤(如环丁烷嘧啶二聚体)的转录和修复在细胞中已被证明是偶联的。转录偶联修复的信号似乎是损伤位点处停滞的转录复合物。为了确定氧化性DNA损伤是否会阻断正确起始的人类RNA聚合酶II,我们检测了位点特异性引入的氧化性损伤对HeLa细胞核提取物中转录的影响。我们发现,当单链断裂(常见的氧化性DNA损伤)存在于转录模板的转录链中时,转录会被阻断。环丁烷嘧啶二聚体先前已被证明在体外和体内均会阻断转录,在HeLa细胞核转录试验中也会阻断转录。相比之下,氧化性DNA碱基损伤8-氧代鸟嘌呤、5-羟基胞嘧啶和胸腺嘧啶乙二醇并不抑制转录,尽管胸腺嘧啶乙二醇损伤会导致停顿。因此,DNA链断裂而非氧化性DNA碱基损伤会阻断RNA聚合酶II的转录。

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