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RecO-mediated DNA homology search and annealing is facilitated by SsbA

机译:利用SsbA促进RecO介导的DNA同源性搜索和退火

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摘要

Bacillus subtilis RecO plays a central role in recombinational repair and genetic recombination by (i) stimulating RecA filamentation onto SsbA-coated single-stranded (ss) DNA, (ii) modulating the extent of RecA-mediated DNA strand exchange and (iii) promoting annealing of complementary DNA strands. Here, we report that RecO-mediated strand annealing is facilitated by cognate SsbA, but not by a heterologous one. Analysis of non-productive intermediates reveals that RecO interacts with SsbA-coated ssDNA, resulting in transient ternary complexes. The self-interaction of ternary complexes via RecO led to the formation of large nucleoprotein complexes. In the presence of homology, SsbA, at the nucleoprotein, removes DNA secondary structures, inhibits spontaneous strand annealing and facilitates RecO loading onto SsbA-ssDNA complex. RecO relieves SsbA inhibition of strand annealing and facilitates transient and random interactions between homologous naked ssDNA molecules. Finally, both proteins lose affinity for duplex DNA. Our results provide a mechanistic framework for rationalizing protein release and dsDNA zippering as coordinated events that are crucial for RecA-independent plasmid transformation.
机译:枯草芽孢杆菌RecO通过(i)将RecA细丝刺激到SsbA包被的单链(ss)DNA上,(ii)调节RecA介导的DNA链交换的程度和(iii)促进重组重组和基因重组中起着核心作用互补DNA链的退火。在这里,我们报告说,RecO介导的链退火是由同源的SsbA促进的,而不是由异源的。对非生产性中间体的分析表明,RecO与SsbA包被的ssDNA相互作用,从而产生瞬时三元复合物。通过RecO的三元复合物的自我相互作用导致形成大的核蛋白复合物。在存在同源性的情况下,核蛋白上的SsbA去除DNA二级结构,抑制自发链退火并促进RecO加载到SsbA-ssDNA复合体上。 RecO减轻了SsbA对链退火的抑制作用,并促进了同源裸ssDNA分子之间的瞬时和随机相互作用。最后,两种蛋白质都失去了对双链DNA的亲和力。我们的结果为合理化蛋白质释放和dsDNA拉链化提供了一个机制框架,这是对独立于RecA的质粒转化至关重要的协调事件。

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