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Synergistic actions of Rad51 and Rad52 in recombination and DNA repair (see comments)

机译:Rad51和Rad52在重组和DNA修复中的协同作用(请参阅评论)

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摘要

In the yeast Saccharomyces cerevisiae, mutations in the genes RAD51 or RAD52 result in severe defects in genetic recombination and the repair of double-strand DNA breaks. These genes, and others of the RAD52 epistasis group (RAD50, RAD54, RAD55, RAD57, RAD59, MRE11 and XRS2), were first identified by their sensitivity to X-rays. They were subsequently shown to be required for spontaneous and induced mitotic recombination, meiotic recombination, and mating-type switching. Human homologues of RAD50, RAD51, RAD52, RAD54 and MRE11 have been identified. Targeted disruption of the murine RAD51 gene results in an embryonic lethal phenotype, indicating that Rad51 protein is required during cell proliferation. Biochemical studies have shown that human RAD51 encodes a protein of relative molecular mass 36,966 (hRad51) that promotes ATP-dependent homologous pairing and DNA strand exchange. As a structural and functional homologue of the RecA protein from Escherichia coli, hRad51 is thought to play a central role in recombination. Yeast Rad51 has been shown to interact with Rad52 protein, as does the human homologue. Here we show that hRad52 stimulates homologous pairing by hRad51. The DNA-binding properties of hRad52 indicate that Rad52 is involved in an early stage of Rad51-mediated recombination.
机译:在酵母酿酒酵母中,基因RAD51或RAD52的突变导致基因重组和双链DNA断裂修复的严重缺陷。这些基因以及RAD52上位性基因组的其他基因(RAD50,RAD54,RAD55,RAD57,RAD59,MRE11和XRS2)首先通过对X射线的敏感性进行鉴定。随后证明它们是自发和诱导的有丝分裂重组,减数分裂重组和交配型转换所必需的。已鉴定出RAD50,RAD51,RAD52,RAD54和MRE11的人类同源物。鼠RAD51基因的靶向破坏导致胚胎致死表型,表明在细胞增殖过程中需要Rad51蛋白。生化研究表明,人RAD51编码相对分子质量为36,966(hRad51)的蛋白质,该蛋白质可促进ATP依赖的同源配对和DNA链交换。作为来自大肠杆菌的RecA蛋白的结构和功能同源物,hRad51被认为在重组中起着核心作用。酵母Rad51已显示与Rad52蛋白相互作用,人类同源物也是如此。在这里,我们显示hRad52刺激hRad51的同源配对。 hRad52的DNA结合特性表明Rad52参与Rad51介导的重组的早期阶段。

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