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细菌DD-肽酶(青霉素结合蛋白)的底物特异性

Substrate specificity of bacterial DD-peptidases (penicillin-binding proteins).

作者信息

Pratt R F

机构信息

Department of Chemistry, Wesleyan University, Lawn Avenue, Middletown, Connecticut 06459, USA.

出版信息

Cell Mol Life Sci. 2008 Jul;65(14):2138-55. doi: 10.1007/s00018-008-7591-7.

Abstract

The DD-peptidase enzymes (penicillin-binding proteins) catalyze the final transpeptidation reaction of bacterial cell wall (peptidoglycan) biosynthesis. Although there is now much structural information available about these enzymes, studies of their activity as enzymes lag. It is now established that representatives of two low-molecular-mass classes of DD-peptidases recognize elements of peptidoglycan structure and rapidly react with substrates and inhibitors incorporating these elements. No members of other DD-peptidase classes, including the high-molecular-mass enzymes, essential for bacterial growth, appear to interact strongly with any particular elements of peptidoglycan structure. Rational design of inhibitors for these enzymes is therefore challenging.

摘要

D-丙氨酰-D-丙氨酸肽酶(青霉素结合蛋白)催化细菌细胞壁(肽聚糖)生物合成的最终转肽反应。尽管现在已有许多关于这些酶的结构信息,但对其酶活性的研究却滞后。现已确定,两类低分子量D-丙氨酰-D-丙氨酸肽酶的代表能够识别肽聚糖结构元件,并与包含这些元件的底物和抑制剂迅速反应。其他D-丙氨酰-D-丙氨酸肽酶类别(包括对细菌生长至关重要的高分子量酶)的成员似乎都不会与肽聚糖结构的任何特定元件发生强烈相互作用。因此,针对这些酶设计抑制剂具有挑战性。

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