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首页> 外文期刊>Molecular & cellular proteomics: MCP >Protein-Protein Interactions Modulate the Docking-Dependent E3-Ubiquitin Ligase Activity of Carboxy-Terminus of Hsc70-Interacting Protein (CHIP).
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Protein-Protein Interactions Modulate the Docking-Dependent E3-Ubiquitin Ligase Activity of Carboxy-Terminus of Hsc70-Interacting Protein (CHIP).

机译:蛋白质-蛋白质相互作用调节Hsc70相互作用蛋白(CHIP)的羧基末端的对接依赖性E3-泛素连接酶活性。

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摘要

CHIP is a tetratricopeptide repeat (TPR) domain protein that functions as an E3-ubiquitin ligase. As well as linking the molecular chaperones to the ubiquitin proteasome system, CHIP also has a docking-dependent mode where it ubiquitinates native substrates, thereby regulating their steady state levels and/or function. Here we explore the effect of Hsp70 on the docking-dependent E3-ligase activity of CHIP. The TPR-domain is revealed as a binding site for allosteric modulators involved in determining CHIP's dynamic conformation and activity. Biochemical, biophysical and modeling evidence demonstrate that Hsp70-binding to the TPR, or Hsp70-mimetic mutations, regulate CHIP-mediated ubiquitination of p53 and IRF-1 through effects on U-box activity and substrate binding. HDX-MS was used to establish that conformational-inhibition-signals extended from the TPR-domain to the U-box. This underscores inter-domain allosteric regulation of CHIP by the core molecular chaperones. Defining the chaperone-associated TPR-domain of CHIP as a manager of inter-domain communication highlights the potential for scaffolding modules to regulate, as well as assemble, complexes that are fundamental to protein homeostatic control.
机译:CHIP是一种四三肽重复(TPR)域蛋白,起E3泛素连接酶的作用。除了将分子伴侣与泛素蛋白酶体系统连接之外,CHIP还具有对接依赖性模式,在该模式下泛素化天然底物,从而调节其稳态水平和/或功能。在这里,我们探讨了Hsp70对CHIP的对接依赖性E3连接酶活性的影响。 TPR结构域被揭示为涉及CHIP动态构象和活性的变构调节剂的结合位点。生化,生物物理和建模证据表明,与TPR结合的Hsp70或Hsp70模拟突变通过影响U-box活性和底物结合来调节CHIP介导的p53和IRF-1泛素化。 HDX-MS用于确定构象抑制信号从TPR域扩展到U-box。这强调了核心分子伴侣对CHIP的域间变构调节。将CHIP的与伴侣相关的TPR域定义为域间通信的管理者,突显了脚手架模块调节和组装对蛋白质稳态控制至关重要的复合物的潜力。

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