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Mechanistic Basis of 5 '-3 ' Translocation in SF1B Helicases

机译:SF1B解旋酶5'-3'易位的机制基础

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摘要

Superfamily 1B (SF1B) helicases translocate in a 5'-3' direction and are required for a range of cellular activities across all domains of life. However, structural analyses to date have focused on how SF1A helicases achieve 3'-5' movement along nucleic acids. We present crystal structures of the complex between the SF1B helicase RecD2 from Deinococcus radiodurans and ssDNA in the presence and absence of an ATP analog. These snapshots of the reaction pathway reveal a nucleotide binding-induced conformational change of the two motor domains that is broadly reminiscent of changes observed in other SF1 and SF2 helicases. Together with biochemical data, the structures point to a step size for translocation of one base per ATP hydrolyzed. Moreover, the structures also reveal a mechanism for nucleic acid translocation in the 5'-3' direction by SF1B helicases that is surprisingly different from that of 3'-5' translocation by SF1A enzymes, and explains the molecular basis of directionality.
机译:超家族1B(SF1B)解旋酶沿5'-3'方向转运,是生命所有领域中一系列细胞活动所必需的。然而,迄今为止的结构分析集中在SF1A解旋酶如何实现沿核酸的3'-5'运动。我们介绍了在存在和不存在ATP类似物的情况下,来自Deinococcus radiodurans的SF1B解旋酶RecD2和ssDNA之间的复合物的晶体结构。反应途径的这些快照揭示了两个运动域的核苷酸结合诱导的构象变化,这广泛地让人联想到在其他SF1和SF2解旋酶中观察到的变化。连同生化数据,结构指向每个ATP水解一个碱基易位的步长。此外,该结构还揭示了通过SF1B解旋酶在5'-3'方向上进行核酸易位的机制,其与通过SF1A酶进行3'-5'易位上的机制令人惊讶地不同,并解释了定向性的分子基础。

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