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H-NS mediates the dissociation of a refractory protein-DNA complex during Tn10/IS10 transposition

机译:H-NS介导Tn10 / IS10转座过程中难治的蛋白质-DNA复合体的解离

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Tn10/IS10 transposition takes place in the context of a protein-DNA complex called a transpososome. During the reaction, the transpososome undergoes several conformational changes. The host proteins IHF and H-NS, which also are global regulators of gene expression, play important roles in directing these architectural changes. IHF binds tightly to only one of two transposon ends within the transpososome, folding this end into a DNA loop structure. Unfolding this DNA loop is necessary for excising the transposon from flanking donor DNA and preventing integration of the transposon into itself. We show here that efficient DNA loop unfolding relies on the continuity of the flanking donor DNA on the side of the transpososome opposite to the folded transposon end. We also show this same donor DNA is a preferred binding site for H-NS, which promotes opening of the IHF-loop, which is required for productive target interactions. This is counter to the usual mode of H-NS action, which is repressive due to its propensity to coat DNA. The interplay between IHF and H-NS likely serves to couple the rate of transposition to the host cell physiology as both of these proteins are integrated into cellular stress response pathways.
机译:Tn10 / IS10转座发生在称为转座体的蛋白质-DNA复合体中。在反应过程中,转座体经历了几种构象变化。宿主蛋白IHF和H-NS也是基因表达的整体调节剂,在指导这些结构变化中起着重要作用。 IHF仅与转座体中两个转座子末端之一紧密结合,将其折叠成DNA环结构。为了使转座子从侧翼供体DNA中切除并防止转座子整合入自身,必须解开该DNA环。我们在这里显示出有效的DNA环展开取决于侧翼供体DNA在转座体与折叠的转座子末端相对的一侧的连续性。我们还显示,相同的供体DNA是H-NS的首选结合位点,可促进IHF环的开放,而IHF环是生产性目标相互作用所必需的。这与H-NS作用的通常模式相反,后者由于具有包覆DNA的倾向而具有抑制作用。 IHF和H-NS之间的相互作用可能有助于将转座速率与宿主细胞生理学联系起来,因为这两种蛋白均已整合到细胞应激反应途径中。

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