8-氧-7,8-二氢鸟嘌呤作用的近距离突变的偏倚分布

IF 1.5 4区 医学 Q4 BIOTECHNOLOGY & APPLIED MICROBIOLOGY Mutation Research-Fundamental and Molecular Mechanisms of Mutagenesis Pub Date : 2022-07-01 DOI:10.1016/j.mrfmmm.2022.111794
Ruriko Fukushima , Tetsuya Suzuki , Yasuo Komatsu , Hiroyuki Kamiya
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引用次数: 1

摘要

8-氧-7,8-二氢鸟嘌呤(8-羟基鸟嘌呤,G°)是一种主要的氧化碱,被认为在包括癌症在内的多种疾病的发病机制中起关键作用。G°诱导损伤位点的G:C→T:A翻转和5 ' -GpA序列上G碱基的非靶向(远距离作用)突变。在这项研究中,我们研究了远距离作用突变的分布以及相对于G°的复制起始位置对非靶向诱变的影响。将G°碱基引入两个穿梭质粒中,每个质粒的SV40复制起点相对于supF基因位于不同的位置。氧化碱基位于义链的上游或下游位点(基因外),或编码基因前trna序列区域的中心。这些穿梭质粒被引入人U2OS细胞。当G°碱基位于supF基因的下游时,远距作用突变比位于该基因的上游时更容易发生。此外,当SV40起源出现在G°碱基的5 '侧时,观察到更多的近距离作用突变。这些结果表明,远距离作用突变主要发生在病变的5 '侧,当受损碱基位于滞后链模板上时发生的频率更高。
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Biased distribution of action-at-a-distance mutations by 8-oxo-7,8-dihydroguanine

8-Oxo-7,8-dihydroguanine (8-hydroxyguanine, G°) is a major oxidized base that is considered to play pivotal roles in the pathogenesis of various diseases, including cancer. G° induces G:C → T:A transversions at the damage site and untargeted (action-at-a-distance) mutations of G bases at 5′-GpA sequences. In this study, we examined the distribution of the action-at-a-distance mutations and the effects of the replication origin position relative to G° on the untargeted mutagenesis. The G° base was introduced into two shuttle plasmids, each with the SV40 replication origin at a different position with respect to the supF gene. The oxidized base was located at an upstream or downstream site (outside of the gene), or the center of the region encoding the pre-tRNA sequence of the gene, in the sense strand. These shuttle plasmids were introduced into human U2OS cells. The action-at-a-distance mutations were more frequently induced when the G° base was located downstream of the supF gene than upstream of the gene. In addition, more action-at-a-distance mutations were observed when the SV40 origin was present on the 5′-side of the G° base. These results indicated that the action-at-a-distance mutations are predominantly induced on the 5′-side of the lesion and occurred more frequently when the damaged base was located on the lagging strand template.

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来源期刊
CiteScore
4.90
自引率
0.00%
发文量
24
审稿时长
51 days
期刊介绍: Mutation Research (MR) provides a platform for publishing all aspects of DNA mutations and epimutations, from basic evolutionary aspects to translational applications in genetic and epigenetic diagnostics and therapy. Mutations are defined as all possible alterations in DNA sequence and sequence organization, from point mutations to genome structural variation, chromosomal aberrations and aneuploidy. Epimutations are defined as alterations in the epigenome, i.e., changes in DNA methylation, histone modification and small regulatory RNAs. MR publishes articles in the following areas: Of special interest are basic mechanisms through which DNA damage and mutations impact development and differentiation, stem cell biology and cell fate in general, including various forms of cell death and cellular senescence. The study of genome instability in human molecular epidemiology and in relation to complex phenotypes, such as human disease, is considered a growing area of importance. Mechanisms of (epi)mutation induction, for example, during DNA repair, replication or recombination; novel methods of (epi)mutation detection, with a focus on ultra-high-throughput sequencing. Landscape of somatic mutations and epimutations in cancer and aging. Role of de novo mutations in human disease and aging; mutations in population genomics. Interactions between mutations and epimutations. The role of epimutations in chromatin structure and function. Mitochondrial DNA mutations and their consequences in terms of human disease and aging. Novel ways to generate mutations and epimutations in cell lines and animal models.
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