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热稳定金属蛋白酶家族中锌金属蛋白酶自身加工的结构基础。

Structural basis for the autoprocessing of zinc metalloproteases in the thermolysin family.

机构信息

State Key Laboratory of Microbial Technology, Marine Biotechnology Research Center, Shandong University, Jinan 250100, China.

出版信息

Proc Natl Acad Sci U S A. 2010 Oct 12;107(41):17569-74. doi: 10.1073/pnas.1005681107. Epub 2010 Sep 27.

Abstract

Thermolysin-like proteases (TLPs), a large group of zinc metalloproteases, are synthesized as inactive precursors. TLPs with a long propeptide (∼200 residues) undergo maturation following autoprocessing through an elusive molecular mechanism. We report the first two crystal structures for the autoprocessed complexes of a typical TLP, MCP-02. In the autoprocessed complex, Ala205 shifts upward by 33 Å from the previously covalently linked residue, His204, indicating that, following autocleavage of the peptide bond between His204 and Ala205, a large conformational change from the zymogen to the autoprocessed complex occurs. The eight N-terminal residues (residues Ala205-Gly212) of the catalytic domain form a new β-strand, nestling into two other β-strands. Simultaneously, the apparent T(m) of the autoprocessed complex increases 20 °C compared to that of the zymogen. The stepwise degradation of the propeptide begins with two sequential cuttings at Ser49-Val50 and Gly57-Leu58, which lead to the disassembly of the propeptide and the formation of mature MCP-02. Our findings give new insights into the molecular mechanism of TLP maturation.

摘要

类糜蛋白酶蛋白酶(TLPs)是一大类锌金属蛋白酶,它们以无活性前体的形式合成。具有长前肽(∼200 个残基)的 TLPs 通过难以捉摸的分子机制自动加工后成熟。我们报告了第一个两个晶体结构为典型的 TLP,MCP-02 的自动加工复合物。在自动加工复合物中,Ala205 从以前共价连接的残基 His204 向上移动 33Å,表明在 His204 和 Ala205 之间的肽键自动切割后,从酶原到自动加工复合物发生了很大的构象变化。催化结构域的前 8 个 N 端残基(残基 Ala205-Gly212)形成一个新的β-链,嵌入到另外两个β-链中。同时,与酶原相比,自动加工复合物的表观 Tm 增加了 20°C。前肽的逐步降解始于 Ser49-Val50 和 Gly57-Leu58 的两个连续切割,这导致前肽的解体和成熟 MCP-02 的形成。我们的发现为 TLP 成熟的分子机制提供了新的见解。

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