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抑制剂结合的封闭态细菌寡肽酶 B 的晶体结构:原生动物和细菌酶之间的相似性和差异。

Crystal Structure of Inhibitor-Bound Bacterial Oligopeptidase B in the Closed State: Similarity and Difference between Protozoan and Bacterial Enzymes.

机构信息

National Research Center "Kurchatov Institute", 123182 Moscow, Russia.

Shemyakin-Ovchinnikov Institute of Bioorganic Chemistry of the Russian Academy of Sciences, 117997 Moscow, Russia.

出版信息

Int J Mol Sci. 2023 Jan 24;24(3):2286. doi: 10.3390/ijms24032286.

Abstract

The crystal structure of bacterial oligopeptidase B from (SpOpB) in complex with a chloromethyl ketone inhibitor was determined at 2.2 Å resolution. SpOpB was crystallized in a closed (catalytically active) conformation. A single inhibitor molecule bound simultaneously to the catalytic residues S532 and H652 mimicked a tetrahedral intermediate of the catalytic reaction. A comparative analysis of the obtained structure and the structure of OpB from (TbOpB) in a closed conformation showed that in both enzymes, the stabilization of the D-loop (carrying the catalytic D) in a position favorable for the formation of a tetrahedral complex occurs due to interaction with the neighboring loop from the β-propeller. However, the modes of interdomain interactions were significantly different for bacterial and protozoan OpBs. Instead of a salt bridge (as in TbOpB), in SpOpB, a pair of polar residues following the catalytic D617 and a pair of neighboring arginine residues from the β-propeller domain formed complementary oppositely charged surfaces. Bioinformatics analysis and structural modeling show that all bacterial OpBs can be divided into two large groups according to these two modes of D-loop stabilization in closed conformations.

摘要

(SpOpB)与氯甲基酮抑制剂复合物的细菌寡肽酶 B 的晶体结构在 2.2Å 分辨率下确定。SpOpB 以封闭(催化活性)构象结晶。一个抑制剂分子同时结合到催化残基 S532 和 H652 上,模拟了催化反应的四面体中间体。对获得的结构和封闭构象的来自 (TbOpB)的 OpB 结构的比较分析表明,在两种酶中,D 环(携带催化 D)的稳定化在有利于形成四面体复合物的位置发生,这是由于与相邻的β-推进器环相互作用所致。然而,细菌和原生动物 OpBs 之间的结构域相互作用模式有很大的不同。在 SpOpB 中,没有形成盐桥(如在 TbOpB 中),而是在催化残基 D617 之后的一对极性残基和β-推进器结构域中的一对相邻精氨酸残基形成互补的相反电荷表面。生物信息学分析和结构建模表明,根据这两种在封闭构象中稳定 D 环的模式,所有细菌 OpB 可以分为两大类。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/47bc/9917282/5e7f852bebd8/ijms-24-02286-g001.jpg

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