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DNA 修复基因:在应对 DNA 损伤剂(电离辐射)时,在exon 水平的转录和基因表达的选择性。

DNA repair genes: alternative transcription and gene expression at the exon level in response to the DNA damaging agent, ionizing radiation.

机构信息

Centre for Innate Immunity and Infectious Disease, Monash Institute for Medical Research, Monash University, Clayton, Victoria, Australia.

出版信息

PLoS One. 2012;7(12):e53358. doi: 10.1371/journal.pone.0053358. Epub 2012 Dec 28.

Abstract

DNA repair is an essential cellular process required to maintain genomic stability. Every cell is subjected to thousands of DNA lesions daily under normal physiological conditions. Ionizing radiation (IR) is a major DNA damaging agent that can be produced by both natural and man-made sources. A common source of radiation exposure is through its use in medical diagnostics or treatments such as for cancer radiotherapy where relatively high doses are received by patients. To understand the detailed DNA repair gene transcription response to high dose IR, gene expression exon array studies have been performed and the response to radiation in two divergent cell types, lymphoblastoid cell lines and primary fibroblasts, has been examined. These exon arrays detect expression levels across the entire gene, and have the advantage of high sensitivity and the ability to identify alternative transcripts. We found a selection of DNA repair genes, including some not previously reported, that are modulated in response to radiation. Detailed dose and time course kinetics of DNA repair transcription was conducted and results have been validated utilizing PCR methods. Alternative transcription products in response to IR were identified in several DNA repair genes including RRM2B and XPC where alternative initiation sites were found. These investigations have advanced the knowledge about the transcriptional response of DNA repair.

摘要

DNA 修复是维持基因组稳定性所必需的细胞过程。在正常生理条件下,每个细胞每天都会受到数千种 DNA 损伤。电离辐射(IR)是一种主要的 DNA 损伤剂,它可以由天然和人为来源产生。辐射暴露的一个常见来源是在医疗诊断或治疗中使用,例如癌症放射治疗,患者会接受相对较高的剂量。为了了解高剂量 IR 对 DNA 修复基因转录的详细反应,已经进行了基因表达外显子阵列研究,并检查了两种不同细胞类型(淋巴母细胞系和原代成纤维细胞)对辐射的反应。这些外显子阵列可以检测整个基因的表达水平,具有高灵敏度和识别替代转录本的优势。我们发现了一些 DNA 修复基因的选择,包括一些以前未报道过的基因,它们会对辐射做出调节。我们进行了 DNA 修复转录的详细剂量和时程动力学研究,并利用 PCR 方法验证了结果。在几个 DNA 修复基因中,包括 RRM2B 和 XPC,发现了对 IR 的替代起始位点,从而鉴定出了替代转录产物。这些研究推进了关于 DNA 修复转录反应的知识。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/6622/3532210/22d15365d562/pone.0053358.g001.jpg

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