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Cul7和PARC保守的CPH结构域是与p53四聚化结构域结合的蛋白质-蛋白质相互作用模块。

The conserved CPH domains of Cul7 and PARC are protein-protein interaction modules that bind the tetramerization domain of p53.

作者信息

Kaustov Lilia, Lukin Jonathan, Lemak Alexander, Duan Shili, Ho Melissa, Doherty Ryan, Penn Linda Z, Arrowsmith Cheryl H

机构信息

Ontario Cancer Institute and the Department of Medical Biophysics, University of Toronto, Ontario, Canada.

出版信息

J Biol Chem. 2007 Apr 13;282(15):11300-7. doi: 10.1074/jbc.M611297200. Epub 2007 Feb 12.

Abstract

Cul7 is a member of the Cullin Ring Ligase (CRL) family and is required for normal mouse development and cellular proliferation. Recently, a region of Cul7 that is highly conserved in the p53-associated, Parkin-like cytoplasmic protein PARC, was shown to bind p53 directly. Here we identify the CPH domains (conserved domain within Cul7, PARC, and HERC2 proteins) of both Cul7 and PARC as p53 interaction domains using size exclusion chromatography and NMR spectroscopy. We present the first structure of the evolutionarily conserved CPH domain and provide novel insight into the Cul7-p53 interaction. The NMR structure of the Cul7-CPH domain reveals a fold similar to peptide interaction modules such as the SH3, Tudor, and KOW domains. The p53 interaction surface of both Cul7 and PARC CPH domains was mapped to a conserved surface distinct from the analogous peptide-binding regions of SH3, KOW, and Tudor domains, suggesting a novel mode of interaction. The CPH domain interaction surface of p53 resides in the tetramerization domain and is formed by residues contributed by at least two subunits.

摘要

Cul7是Cullin环连接酶(CRL)家族的成员,是正常小鼠发育和细胞增殖所必需的。最近,在与p53相关的、Parkin样细胞质蛋白PARC中高度保守的Cul7区域被证明可直接结合p53。在这里,我们使用尺寸排阻色谱法和核磁共振光谱法将Cul7和PARC的CPH结构域(Cul7、PARC和HERC2蛋白中的保守结构域)鉴定为p53相互作用结构域。我们展示了进化上保守的CPH结构域的首个结构,并为Cul7-p53相互作用提供了新的见解。Cul7-CPH结构域的核磁共振结构揭示了一种与肽相互作用模块(如SH3、Tudor和KOW结构域)相似的折叠。Cul7和PARC CPH结构域的p53相互作用表面被定位到一个与SH3、KOW和Tudor结构域的类似肽结合区域不同的保守表面,这表明了一种新的相互作用模式。p53的CPH结构域相互作用表面位于四聚化结构域中,由至少两个亚基贡献的残基形成。

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