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人类胆碱乙酰转移酶的底物结合与催化机制

Substrate binding and catalytic mechanism of human choline acetyltransferase.

作者信息

Kim Ae-Ri, Rylett R Jane, Shilton Brian H

机构信息

Department of Biochemistry, and Physiology and Pharmacology, Schulich School of Medicine and Dentistry, University of Western Ontario, Ontario, Canada.

出版信息

Biochemistry. 2006 Dec 12;45(49):14621-31. doi: 10.1021/bi061536l.

Abstract

Choline acetyltransferase (ChAT) catalyzes the synthesis of the neurotransmitter acetylcholine from choline and acetyl-CoA, and its presence is a defining feature of cholinergic neurons. We report the structure of human ChAT to a resolution of 2.2 A along with structures for binary complexes of ChAT with choline, CoA, and a nonhydrolyzable acetyl-CoA analogue, S-(2-oxopropyl)-CoA. The ChAT-choline complex shows which features of choline are important for binding and explains how modifications of the choline trimethylammonium group can be tolerated by the enzyme. A detailed model of the ternary Michaelis complex fully supports the direct transfer of the acetyl group from acetyl-CoA to choline through a mechanism similar to that seen in the serine hydrolases for the formation of an acyl-enzyme intermediate. Domain movements accompany CoA binding, and a surface loop, which is disordered in the unliganded enzyme, becomes localized and binds directly to the phosphates of CoA, stabilizing the complex. Interactions between this surface loop and CoA may function to lower the KM for CoA and could be important for phosphorylation-dependent regulation of ChAT activity.

摘要

胆碱乙酰转移酶(ChAT)催化由胆碱和乙酰辅酶A合成神经递质乙酰胆碱,其存在是胆碱能神经元的一个决定性特征。我们报告了分辨率为2.2埃的人ChAT的结构,以及ChAT与胆碱、辅酶A和一种不可水解的乙酰辅酶A类似物S-(2-氧代丙基)-辅酶A的二元复合物的结构。ChAT-胆碱复合物显示了胆碱的哪些特征对结合很重要,并解释了胆碱三甲基铵基团的修饰如何能被该酶耐受。三元米氏复合物的详细模型完全支持乙酰基团从乙酰辅酶A直接转移到胆碱,其机制类似于丝氨酸水解酶中形成酰基-酶中间体的机制。结构域运动伴随辅酶A结合,并且一个在未结合配体的酶中无序的表面环变得定位并直接结合到辅酶A的磷酸基团上,从而稳定复合物。这个表面环与辅酶A之间的相互作用可能起到降低辅酶A的米氏常数的作用,并且可能对ChAT活性的磷酸化依赖性调节很重要。

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