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An 'open' structure of the RecOR complex supports ssDNA binding within the core of the complex

机译:RecOR复合物的“开放”结构支持复合物核心内的ssDNA结合

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摘要

Efficient DNA repair is critical for cell survival and the maintenance of genome integrity. The homologous recombination pathway is responsible for the repair of DNA double-strand breaks within cells. Initiation of this pathway in bacteria can be carried out by either the RecBCD or the RecFOR proteins. An important regulatory player within the RecFOR pathway is the RecOR complex that facilitates RecA loading onto DNA. Here we report new data regarding the assembly of Deinococcus radiodurans RecOR and its interaction with DNA, providing novel mechanistic insight into the mode of action of RecOR in homologous recombination. We present a higher resolution crystal structure of RecOR in an 'open' conformation in which the tetrameric RecR ring flanked by two RecO molecules is accessible for DNA binding. We show using small-angle neutron scattering and mutagenesis studies that DNA binding does indeed occur within the RecR ring. Binding of single-stranded DNA occurs without any major conformational changes of the RecOR complex while structural rearrangements are observed on double-stranded DNA binding. Finally, our molecular dynamics simulations, supported by our biochemical data, provide a detailed picture of the DNA binding motif of RecOR and reveal that single-stranded DNA is sandwiched between the two facing oligonucleotide binding domains of RecO within the RecR ring.
机译:高效的DNA修复对于细胞存活和基因组完整性的维持至关重要。同源重组途径负责修复细胞内DNA双链断裂。 RecBCD或RecFOR蛋白均可在细菌中启动此途径。 RecFOR途径中一个重要的调控因素是RecOR复合物,它有助于RecA加载到DNA上。在这里,我们报告有关Deinococcus radiodurans RecOR的装配及其与DNA相互作用的新数据,为RecOR在同源重组中的作用方式提供了新颖的机理见解。我们提出了一个'开放'构象中的RecOR的更高分辨率的晶体结构,其中两侧是两个RecO分子的四聚RecR环可用于DNA结合。我们使用小角度中子散射和诱变研究表明,RecR环内确实发生了DNA结合。单链DNA的结合没有RecOR复杂的任何主要构象变化,而在双链DNA结合上观察到结构重排。最后,在生物化学数据的支持下,我们的分子动力学模拟提供了RecOR DNA结合基序的详细图片,并揭示了单链DNA夹在RecR环内RecO的两个相对的寡核苷酸结合结构域之间。

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