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Structural basis of ubiquitin recognition by the winged-helix domain of Cockayne syndrome group B protein

机译:Cockayne综合征B组蛋白的有翼螺旋结构域识别遍在蛋白的结构基础

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摘要

Cockayne syndrome group B (CSB, also known as ERCC6) protein is involved in many DNA repair processes and essential for transcription-coupled repair (TCR). The central region of CSB has the helicase motif, whereas the C-terminal region contains important regulatory elements for repair of UV- and oxidative stress-induced damages and double-strand breaks (DSBs). A previous study suggested that a small part (∼30 residues) within this region was responsible for binding to ubiquitin (Ub). Here, we show that the Ub-binding of CSB requires a larger part of CSB, which was previously identified as a winged-helix domain (WHD) and is involved in the recruitment of CSB to DSBs. We also present the crystal structure of CSB WHD in complex with Ub. CSB WHD folds as a single globular domain, defining a class of Ub-binding domains (UBDs) different from 23 UBD classes identified so far. The second α-helix and C-terminal extremity of CSB WHD interact with Ub. Together with structure-guided mutational analysis, we identified the residues critical for the binding to Ub. CSB mutants defective in the Ub binding reduced repair of UV-induced damage. This study supports the notion that DSB repair and TCR may be associated with the Ub-binding of CSB.
机译:Cockayne综合征B组(CSB,也称为ERCC6)蛋白参与许多DNA修复过程,是转录偶联修复(TCR)所必需的。 CSB的中央区域具有解旋酶基序,而C末端区域包含重要的调控元件,可修复UV和氧化应激诱导的损伤和双链断裂(DSB)。先前的研究表明,该区域中的一小部分(约30个残基)与泛素(Ub)结合。在这里,我们显示CSB的Ub绑定需要CSB的较大部分,而CSB先前被确定为有翼螺旋域(WHD),并且涉及CSB向DSB的募集。我们还介绍了与Ub复合的CSB WHD的晶体结构。 CSB WHD折叠为单个球状域,从而定义了一类Ub结合域(UBD),与迄今确定的23个UBD类不同。 CSB WHD的第二个α螺旋和C末端与Ub相互作用。结合结构指导的突变分析,我们确定了与Ub结合至关重要的残基。 Ub结合缺陷的CSB突变体减少了UV诱导的损伤的修复。这项研究支持DSB修复和TCR可能与CSB的Ub结合有关的观点。

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