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Hdf1是一种酵母Ku蛋白同源物,参与非同源重组,但不参与同源重组。

Hdf1, a yeast Ku-protein homologue, is involved in illegitimate recombination, but not in homologous recombination.

作者信息

Tsukamoto Y, Kato J, Ikeda H

机构信息

Department of Molecular Biology, Institute of Medical Science, University of Tokyo, Japan.

出版信息

Nucleic Acids Res. 1996 Jun 1;24(11):2067-72. doi: 10.1093/nar/24.11.2067.

Abstract

Hdf1 is the yeast homologue of the mammalian 70 kDa subunit of Ku-protein, which has DNA end-binding activity and is involved in DNA double-strand break repair and V(D)J recombination. To examine whether Hdf1 is involved in illegitimate recombination, we have measured the rate of deletion mutation caused by illegitimate recombination on a plasmid in an hdf1 disruptant. The hdf1 mutation reduced the rate of deletion formation by 20-fold, while it did not affect mitotic and meiotic homologous recombinations between two heteroalleles or homologous recombination between direct repeats. Hence Hdf1 participates in illegitimate recombination, but not in homologous recombination, in contrast to Rad52, Rad50, Mre11 and Xrs2, which are involved in both homologous and illegitimate recombination. The illegitimate recombination in the hdf1 disruptant took place between recombination sites that shared short regions of homology (1-4 bp), as was observed in the wild-type. Based on the DNA end-binding activity of Hdf1, we discuss models in which Hdf1 plays an important role in the late step of illegitimate recombination.

摘要

Hdf1是哺乳动物Ku蛋白70 kDa亚基的酵母同源物,具有DNA末端结合活性,参与DNA双链断裂修复和V(D)J重组。为了检测Hdf1是否参与异常重组,我们测定了hdf1缺陷型中质粒上由异常重组引起的缺失突变率。hdf1突变使缺失形成率降低了20倍,而它不影响两个异等位基因之间的有丝分裂和减数分裂同源重组或同向重复序列之间的同源重组。因此,与参与同源重组和异常重组的Rad52、Rad50、Mre11和Xrs2不同,Hdf1参与异常重组,但不参与同源重组。在hdf1缺陷型中,异常重组发生在具有短同源区域(1-4 bp)的重组位点之间,这与野生型中观察到的情况相同。基于Hdf1的DNA末端结合活性,我们讨论了Hdf1在异常重组后期发挥重要作用的模型。

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