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从结核分枝杆菌ClpP1的X射线结构洞察酪蛋白水解蛋白酶的环间可塑性。

Insights into the inter-ring plasticity of caseinolytic proteases from the X-ray structure of Mycobacterium tuberculosis ClpP1.

作者信息

Ingvarsson Henrik, Maté María J, Högbom Martin, Portnoï Denis, Benaroudj Nadia, Alzari Pedro M, Ortiz-Lombardía Miguel, Unge Torsten

机构信息

Department of Cell and Molecular Biology, Uppsala University, Biomedical Center, Box 596, SE-751 24 Uppsala, Sweden.

出版信息

Acta Crystallogr D Biol Crystallogr. 2007 Feb;63(Pt 2):249-59. doi: 10.1107/S0907444906050530. Epub 2007 Jan 16.

DOI:10.1107/S0907444906050530
PMID:17242518
Abstract

Mycobacterium tuberculosis caseinolytic protease ClpP1 (Mt ClpP1) is a self-compartmentalized protease consisting of two heptameric rings stacked on top of each other, thus enclosing a catalytic chamber. Within the chamber, which can be reached through two axial pores, each of the 14 identical monomers possesses a serine protease active site. The unfolding and translocation of substrates into the chamber are mediated by associated hexameric ATPases covering the axial pores. Three crystal structures of Mt ClpP1, determined by molecular replacement, are presented in this study. Two of the models were refined to a resolution of 2.6 A and the third to 3.0 A. It was found that disorder in the handle domain affects the formation and configuration of the tetradecamer and results in condensed structures with larger equatorial pores when compared with ClpPs from other species. Additionally, this disorder accompanies conformational changes of the residues in the catalytic triad. The models also reveal structural differences within the N-terminal hairpin-loop domain, which possibly reflect the significant differences in amino-acid sequence between Mt ClpP1 and other ClpP homologues in this region.

摘要

结核分枝杆菌酪蛋白水解蛋白酶ClpP1(Mt ClpP1)是一种自我分隔的蛋白酶,由两个相互堆叠的七聚体环组成,从而围成一个催化腔室。在该腔室内,可通过两个轴向孔进入,14个相同的单体中的每一个都具有一个丝氨酸蛋白酶活性位点。底物的解折叠和转运到腔室中是由覆盖轴向孔的相关六聚体ATP酶介导的。本研究展示了通过分子置换确定的Mt ClpP1的三种晶体结构。其中两个模型被精修至2.6 Å的分辨率,第三个模型被精修至3.0 Å的分辨率。研究发现,柄结构域的无序状态会影响十四聚体的形成和构象,与其他物种的ClpP相比,会导致赤道孔较大的致密结构。此外,这种无序状态伴随着催化三联体中残基的构象变化。这些模型还揭示了N端发夹环结构域内的结构差异,这可能反映了Mt ClpP1与该区域其他ClpP同源物在氨基酸序列上的显著差异。

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