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捕获β-糖苷酶上的共价中间体。

Trapping covalent intermediates on beta-glycosidases.

作者信息

Wicki Jacqueline, Rose David R, Withers Stephen G

机构信息

Department of Chemistry, University of British Columbia, Vancouver, British Columbia, Canada V6T 1Z1.

出版信息

Methods Enzymol. 2002;354:84-105. doi: 10.1016/s0076-6879(02)54007-6.

Abstract

The mechanism-based inactivation and subsequent identification of the nucleophilic residue using mass spectrometry have been successfully applied and used to identify the active-site nucleophile in numerous beta-glycosidases, as illustrated using C. fimi exoglycanase. Evidence for a covalent glycosyl-enzyme intermediate has come from X-ray crystallographic analysis of trapped complexes, the first being that of the trapped fluoroglycosyl-enzyme intermediate of Cex. The crystal structure of the trapped fluorocellobiosyl-enzyme complex for Cex has provided useful insights into catalysis and the roles of specific residues at the active site. In addition, information about the conformation of the natural sugar in the covalently bound state and the interactions at the active site was obtained using a mutant form of Cex.

摘要

基于机制的失活以及随后使用质谱法鉴定亲核残基,已成功应用于众多β-糖苷酶中活性位点亲核试剂的鉴定,如使用嗜纤维梭菌外切聚糖酶所展示的那样。共价糖基-酶中间体的证据来自对捕获复合物的X射线晶体学分析,第一个是Cex捕获的氟糖基-酶中间体的分析。Cex捕获的氟纤维二糖基-酶复合物的晶体结构为催化作用以及活性位点特定残基的作用提供了有用的见解。此外,使用Cex的突变形式获得了关于共价结合状态下天然糖的构象以及活性位点相互作用的信息。

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