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WDR20 调节 USP12 x UAF1 去泛素化酶复合物的活性。

WDR20 regulates activity of the USP12 x UAF1 deubiquitinating enzyme complex.

机构信息

Department of Radiation Oncology, Dana-Farber Cancer Institute, Boston, Massachusetts 02115, USA.

出版信息

J Biol Chem. 2010 Apr 9;285(15):11252-7. doi: 10.1074/jbc.M109.095141. Epub 2010 Feb 10.

Abstract

The UAF1 (Usp1-associated factor 1) protein binds and stimulates three deubiquitinating enzymes: USP1, USP12, and USP46. Although the USP1 x UAF1 complex is required for regulation of the Fanconi anemia (FA) DNA repair pathway, less is known about the USP12 x UAF1 and the USP46 x UAF1 complexes. To understand further the nature of the USP12 and USP46 complexes, we attempted to identify proteins that interact with the USP12 and USP46 deubiquitinating enzyme complexes. We identified WDR20, a WD40-repeat containing protein, as a common binding partner of UAF1, USP12, and USP46. Further analysis showed that WDR20 associates exclusively with USP12 and USP46, not with USP1. Furthermore, we demonstrate the purification of a ternary USP12 x UAF1 x WDR20 complex. Interestingly, and consistent with the binding assays, WDR20 stimulated the enzymatic activity of USP12 x UAF1, but not of USP1 x UAF1. Consistent with our previous report that USP12 and USP46 do not regulate the FA pathway, small interference RNA-mediated depletion of WDR20 protein did not affect the FA pathway or DNA damage responses. We provide a model in which WDR20 serves as a stimulatory subunit for preserving and regulating the activity of the subset of the UAF1 x USP complexes.

摘要

UAF1(Usp1 相关因子 1)蛋白结合并刺激三种去泛素化酶:USP1、USP12 和 USP46。尽管 USP1 x UAF1 复合物是调节范可尼贫血(FA)DNA 修复途径所必需的,但对于 USP12 x UAF1 和 USP46 x UAF1 复合物的了解较少。为了进一步了解 USP12 和 USP46 复合物的性质,我们试图鉴定与 USP12 和 USP46 去泛素化酶复合物相互作用的蛋白质。我们鉴定出 WDR20 是一种含有 WD40 重复序列的蛋白质,它是 UAF1、USP12 和 USP46 的共同结合伴侣。进一步的分析表明,WDR20 仅与 USP12 和 USP46 相关联,而与 USP1 无关。此外,我们还证明了 USP12 x UAF1 x WDR20 三元复合物的纯化。有趣的是,与结合测定结果一致,WDR20 刺激了 USP12 x UAF1 的酶活性,但不刺激 USP1 x UAF1 的酶活性。与我们之前的报告一致,USP12 和 USP46 不调节 FA 途径,因此 WDR20 蛋白的小干扰 RNA 介导耗尽不会影响 FA 途径或 DNA 损伤反应。我们提出了一个模型,其中 WDR20 作为一个刺激亚基,用于维持和调节 UAF1 x USP 复合物亚组的活性。

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