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Direct association of Bloom's syndrome gene product with the human mismatch repair protein MLH1

机译:Bloom综合征基因产物与人类错配修复蛋白MLH1直接关联

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摘要

Bloom's syndrome (BS) is a rare genetic disorder characterised by genomic instability and cancer susceptibility. BLM, the gene mutated in BS, encodes a member of the RecQ family of DNA helicases. Here, we identify hMLH1, which is involved in mismatch repair (MMR) and recombination, as a protein that directly interacts with BLM both in vivo and in vitro, and that the two proteins co-localise to discrete nuclear foci. The interaction between BLM and hMLH1 appears to have been evolutionarily conserved, as Sgs1p, the Saccharomyces cerevisiae homologue of BLM, interacts with yeast Mlh1p. However, cell extracts derived from BS patients show no obvious defects in MMR compared to wild-type- and BLM-complemented BS cell extracts. We conclude that the hMLH1-BLM interaction is not essential for post-replicative MMR, but, more likely, is required for some aspect of genetic recombination
机译:布鲁姆综合症(BS)是一种罕见的遗传疾病,其特征是基因组不稳定和癌症易感性。 BLM是在BS中突变的基因,它编码DNA解旋酶RecQ家族的成员。在这里,我们确定参与错配修复(MMR)和重组的hMLH1是一种在体内和体外均可直接与BLM相互作用的蛋白质,并且这两种蛋白质共同定位于离散的核灶。 BLM和hMLH1之间的相互作用似乎在进化上是保守的,因为BLM的酿酒酵母同源物Sgs1p与酵母Mlh1p相互作用。但是,与野生型和BLM互补的BS细胞提取物相比,来自BS患者的细胞提取物在MMR中没有显示出明显的缺陷。我们得出的结论是,hMLH1-BLM相互作用对于复制后的MMR并不是必不可少的,但更可能是基因重组的某些方面所必需的

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