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Rpt1p 与 26S 蛋白酶体特有伴侣蛋白 Hsm3p 特异性识别的结构基础。Rpt1p 是 26S 蛋白酶体的 ATP 酶亚基。

Structural basis for specific recognition of Rpt1p, an ATPase subunit of 26 S proteasome, by proteasome-dedicated chaperone Hsm3p.

机构信息

Picobiology Institute, Department of Life Science, Graduate School of Life Science, University of Hyogo, 3-2-1, Kouto, Kamigori-cho, Ako-gun, Hyogo, 678-1297, Japan.

出版信息

J Biol Chem. 2012 Apr 6;287(15):12172-82. doi: 10.1074/jbc.M112.345876. Epub 2012 Feb 8.

DOI:10.1074/jbc.M112.345876
PMID:22334676
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3320968/
Abstract

The 26 S proteasome is a 2.5-MDa molecular machine that degrades ubiquitinated proteins in eukaryotic cells. It consists of a proteolytic core particle and two 19 S regulatory particles (RPs) composed of 6 ATPase (Rpt) and 13 non-ATPase (Rpn) subunits. Multiple proteasome-dedicated chaperones facilitate the assembly of the proteasome, but little is known about the detailed mechanisms. Hsm3, a 19 S RP dedicated chaperone, transiently binds to the C-terminal domain of the Rpt1 subunit and forms a tetrameric complex, Hsm3-Rpt1-Rpt2-Rpn1, during maturation of the ATPase ring of 19 S RP. To elucidate the structural basis of Hsm3 function, we determined the crystal structures of Hsm3 and its complex with the C-terminal domain of the Rpt1 subunit (Rpt1C). Hsm3 has a C-shaped structure that consists of 11 HEAT repeats. The structure of the Hsm3-Rpt1C complex revealed that the interacting surface between Hsm3 and Rpt1 is a hydrophobic core and a complementary charged surface. Mutations in the Hsm3-Rpt1 surface resulted in the assembly defect of the 26 S proteasome. Furthermore, a structural model of the Hsm3-Rpt ring complex and an in vitro binding assay suggest that Hsm3 can bind Rpt2 in addition to Rpt1. Collectively, our results provide the structural basis of the molecular functions of Hsm3 for the RP assembly.

摘要

26S 蛋白酶体是一种 2.5MDa 的分子机器,可在真核细胞中降解泛素化的蛋白质。它由一个蛋白酶核心颗粒和两个由 6 个 ATP 酶(Rpt)和 13 个非 ATP 酶(Rpn)亚基组成的 19S 调节颗粒(RP)组成。多种蛋白酶体专用伴侣蛋白促进蛋白酶体的组装,但对其详细机制知之甚少。Hsm3 是一种 19S RP 专用伴侣蛋白,在 19S RP 的 ATP 酶环成熟过程中,它会与 Rpt1 亚基的 C 末端结构域短暂结合,并形成一个四聚体复合物 Hsm3-Rpt1-Rpt2-Rpn1。为了阐明 Hsm3 功能的结构基础,我们测定了 Hsm3 及其与 Rpt1 C 末端结构域(Rpt1C)复合物的晶体结构。Hsm3 具有 C 形结构,由 11 个 HEAT 重复序列组成。Hsm3-Rpt1C 复合物的结构表明,Hsm3 和 Rpt1 之间的相互作用表面是一个疏水性核心和一个互补的带电表面。Hsm3 和 Rpt1 表面的突变导致 26S 蛋白酶体的组装缺陷。此外,Hsm3-Rpt 环复合物的结构模型和体外结合测定表明,Hsm3 除了可以结合 Rpt1 之外,还可以结合 Rpt2。总的来说,我们的结果为 Hsm3 对 RP 组装的分子功能提供了结构基础。

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