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α-胰凝乳蛋白酶激活的模拟:前肽的途径及作用分析

Simulation of the activation of alpha-chymotrypsin: analysis of the pathway and role of the propeptide.

作者信息

Mátrai Janka, Verheyden Gert, Krüger Peter, Engelborghs Yves

机构信息

Laboratory of Biomolecular Dynamics, Katholieke Universiteit Leuven, B-3001 Leuven, Belgium.

出版信息

Protein Sci. 2004 Dec;13(12):3139-50. doi: 10.1110/ps.04825004.

Abstract

Alpha-chymotrypsin undergoes a reversible conformational change from an inactive chymotrypsinogen-like structure at high pH to an active conformation at neutral pH. In order to gain insight into this process on a structural level, we applied molecular dynamics and targeted molecular dynamics simulations in aqueous environment on the activation and inactivation processes of three different types of chymotrypsin. These are the wild-type bovine chymotrypsin containing the propeptide and the bovine and rat chymotrypsin lacking the propeptide. From these simulations, the importance of the propeptide and of the sequence differences between the rat and bovine variants from the viewpoint of activation could be evaluated and compared with previous fluorescence stopped flow results. The obtained results show the unambiguous influence of the propeptide on the explored conformational space, whereas the sequence differences between bovine and rat chymotrypsin play a minor role. The main features of activation are present in both the wild type and the variant lacking the propeptide, despite the fact that different parts of the conformational space were explored. The comparison of all trajectories shows that particular amino acid residues, such as 17, 18, 19, 187, 217, 218, and 223, undergo large dihedral transitions during the activation process, suggesting a role as hinge residues during the conformational change.

摘要

α-胰凝乳蛋白酶经历从高pH下无活性的胰凝乳蛋白酶原样结构到中性pH下活性构象的可逆构象变化。为了在结构层面深入了解这一过程,我们在水环境中对三种不同类型的胰凝乳蛋白酶的激活和失活过程应用了分子动力学和靶向分子动力学模拟。这三种类型分别是含有前肽的野生型牛胰凝乳蛋白酶以及缺乏前肽的牛和大鼠胰凝乳蛋白酶。通过这些模拟,可以从激活的角度评估前肽以及大鼠和牛变体之间序列差异的重要性,并与先前的荧光停流结果进行比较。所得结果表明前肽对所探索的构象空间有明确影响,而牛和大鼠胰凝乳蛋白酶之间的序列差异作用较小。尽管探索的是构象空间的不同部分,但激活的主要特征在野生型和缺乏前肽的变体中均存在。对所有轨迹的比较表明,特定的氨基酸残基,如17、18、19、187、217、218和223,在激活过程中经历大的二面角转变,表明它们在构象变化过程中作为铰链残基发挥作用。

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