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XBP-Bax1 解旋酶-核酸酶复合物解开并切割 DNA:对真核生物和古菌核苷酸切除修复的影响。

The XBP-Bax1 helicase-nuclease complex unwinds and cleaves DNA: implications for eukaryal and archaeal nucleotide excision repair.

机构信息

Centre for Biomolecular Sciences, University of St. Andrews, North Haugh, Fife KY16 9ST, Scotland, United Kingdom.

出版信息

J Biol Chem. 2010 Apr 2;285(14):11013-22. doi: 10.1074/jbc.M109.094763. Epub 2010 Feb 6.

Abstract

XPB helicase is an integral part of transcription factor TFIIH, required for both transcription initiation and nucleotide excision repair (NER). Along with the XPD helicase, XPB plays a crucial but only partly understood role in defining and extending the DNA repair bubble around lesions in NER. Archaea encode clear homologues of XPB and XPD, and structural studies of these proteins have yielded key insights relevant to the eukaryal system. Here we show that archaeal XPB functions with a structure-specific nuclease, Bax1, as a helicase-nuclease machine that unwinds and cleaves model NER substrates. DNA bubbles are extended by XPB and cleaved by Bax1 at a position equivalent to that cut by the XPG nuclease in eukaryal NER. The helicase activity of archaeal XPB is dependent on the conserved Thumb domain, which may act as the helix breaker. The N-terminal damage recognition domain of XPB is shown to be crucial for XPB-Bax1 activity and may be unique to the archaea. These findings have implications for the role of XPB in both archaeal and eukaryal NER and for the evolution of the NER pathway. XPB is shown to be a very limited helicase that can act on small DNA bubbles and open a defined region of the DNA duplex. The specialized functions of the accessory domains of XPB are now more clearly delineated. This is also the first direct demonstration of a repair function for archaeal XPB and suggests strongly that the role of XPB in transcription occurred later in evolution than that in repair.

摘要

XPB 解旋酶是转录因子 TFIIH 的一个组成部分,对于转录起始和核苷酸切除修复(NER)都必不可少。与 XPD 解旋酶一起,XPB 在定义和扩展 NER 中损伤周围的 DNA 修复泡方面发挥着至关重要但部分未知的作用。古菌编码了 XPB 和 XPD 的清晰同源物,这些蛋白质的结构研究为真核系统提供了关键的见解。在这里,我们表明古菌 XPB 与结构特异性核酸酶 Bax1 一起作为解旋酶-核酸酶机器,可解旋和切割 NER 模型底物。XPB 扩展 DNA 泡,并由 Bax1 在与真核 NER 中 XPG 核酸酶切割位置等效的位置切割。古菌 XPB 的解旋酶活性依赖于保守的拇指结构域,该结构域可能作为螺旋断裂酶。XPB 的 N 端损伤识别结构域对于 XPB-Bax1 活性至关重要,并且可能是古菌所特有的。这些发现对 XPB 在古菌和真核 NER 中的作用以及 NER 途径的进化具有重要意义。XPB 被证明是一种非常有限的解旋酶,它可以作用于小 DNA 泡并打开 DNA 双链的特定区域。现在,XPB 辅助结构域的特殊功能更加明确。这也是首次直接证明古菌 XPB 的修复功能,强烈表明 XPB 在转录中的作用比在修复中的作用在进化上出现得更晚。

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