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首页> 外文期刊>Nucleic acids research >Interactions between BRCA2 and RAD51 for promoting homologous recombination in Leishmania infantum
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Interactions between BRCA2 and RAD51 for promoting homologous recombination in Leishmania infantum

机译:BRCA2和RAD51之间的相互作用促进婴儿利什曼原虫的同源重组

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摘要

In most organisms, the primary function of homologous recombination (HR) is to allow genome protection by the faithful repair of DNA double-strand breaks. The vital step of HR is the search for sequence homology, mediated by the RAD51 recombinase, which is stimulated further by proteins mediators such as the tumor suppressor BRCA2. The biochemical interplay between RAD51 and BRCA2 is unknown in Leishmania or Trypanosoma. Here we show that the Leishmania infantum BRCA2 protein possesses several critical features important for the regulation of DNA recombination at the genetic and biochemical level. A BRCA2 null mutant, generated by gene disruption, displayed genomic instability and gene-targeting defects. Furthermore, cytological studies show that LiRAD51 can no longer localize to the nucleus in this mutant. The Leishmania RAD51 and BRCA2 interact together and the purified proteins bind single-strand DNA. Remarkably, LiBRCA2 is a recombination mediator that stimulates the invasion of a resected DNA double-strand break in an undamaged template by LiRAD51 to form a D-loop structure. Collectively, our data show that LiBRCA2 and LiRAD51 promote HR at the genetic and biochemical level in L. infantum, the causative agent of visceral leishmaniasis.
机译:在大多数生物中,同源重组(HR)的主要功能是通过忠实修复DNA双链断裂来保护基因组。 HR的重要步骤是寻找由RAD51重组酶介导的序列同源性,而该同源性又被诸如肿瘤抑制物BRCA2之类的蛋白质介体进一步刺激。在利什曼原虫或锥虫中,RAD51和BRCA2之间的生化相互作用是未知的。在这里,我们显示婴儿利什曼原虫BRCA2蛋白具有几个重要的特征,这些特征对于在基因和生化水平上的DNA重组调控至关重要。由基因破坏产生的BRCA2空突变体显示出基因组不稳定和基因靶向缺陷。此外,细胞学研究表明,该突变体中LiRAD51不再能定位于细胞核。利什曼原虫RAD51和BRCA2相互作用,纯化的蛋白质结合单链DNA。值得注意的是,LiBRCA2是重组介体,可通过LiRAD51刺激未损伤模板中的切除DNA双链断裂的入侵,形成D环结构。总体而言,我们的数据表明LiBRCA2和LiRAD51在内生利什曼病的病原体婴儿乳杆菌的遗传和生化水平上促进了HR。

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