首页> 美国卫生研究院文献>Genetics >Efficient repair of all types of single-base mismatches in recombination intermediates in Chinese hamster ovary cells. Competition between long-patch and G-T glycosylase-mediated repair of G-T mismatches.
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Efficient repair of all types of single-base mismatches in recombination intermediates in Chinese hamster ovary cells. Competition between long-patch and G-T glycosylase-mediated repair of G-T mismatches.

机译:有效修复中国仓鼠卵巢细胞重组中间体中所有类型的单碱基错配。长补丁和G-T糖基化酶介导的G-T错配修复之间的竞争。

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摘要

Repair of all 12 single-base mismatches in recombination intermediates was investigated in Chinese hamster ovary cells. Extrachromosomal recombination was stimulated by double-strand breaks in regions of shared homology. Recombination was predicted to occur via single-strand annealing, yielding heteroduplex DNA (hDNA) with a single mismatch. Nicks were expected on opposite strands flanking hDNA, equidistant from the mismatch. Unlike studies of covalently closed artificial hDNA substrates, all mismatches were efficiently repaired, consistent with a nick-driven repair process. The average repair efficiency for all mispairs was 92%, with no significant differences among mispairs. There was significant strand-independent repair of G-T --> G-C, with a slightly greater bias in a CpG context. Repair of C-A was also biased (toward C-G), but no A-C --> G-C bias was found, a possible sequence context effect. No other mismatches showed evidence of biased repair, but among hetero-mismatches, the trend was toward retention of C or G vs. A or T. Repair of both T-T and G-T mismatches was much less efficient in mismatch repair-deficient cells (approximately 25%), and the residual G-T repair was completely biased toward G-C. Our data indicate that single-base mismatches in recombination intermediates are substrates for at least two competing repair systems.
机译:在中国仓鼠卵巢细胞中研究了重组中间体中所有12个单碱基错配的修复。共有同源区域中的双链断裂刺激了染色体外重组。重组预计通过单链退火发生,产生具有单个错配的异源双链DNA(hDNA)。预期在与错配等距的hDNA侧翼的相反链上有缺口。与共价封闭的人工hDNA底物的研究不同,所有错配都得到了有效修复,与缺口驱动的修复过程一致。所有故障配对的平均修复效率为92%,故障配对之间无显着差异。 G-T-> G-C发生了显着的链独立修复,在CpG情况下偏倚稍大。 C-A的修复也有偏见(朝向C-G),但未发现A-C-> G-C偏见,这可能是序列上下文效应。没有其他错配显示出修复有偏见的证据,但是在异质错配中,趋势是趋向于保留C或G与A或T。在错配修复缺陷的细胞中,TT和GT错配的修复效率要低得多(大约25 %),而剩余的GT修复完全偏向GC。我们的数据表明,重组中间体中的单碱基错配是至少两个竞争性修复系统的底物。

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