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认识到蛋白质连接聚糖是肽酶活性的一个决定因素。

Recognition of protein-linked glycans as a determinant of peptidase activity.

作者信息

Noach Ilit, Ficko-Blean Elizabeth, Pluvinage Benjamin, Stuart Christopher, Jenkins Meredith L, Brochu Denis, Buenbrazo Nakita, Wakarchuk Warren, Burke John E, Gilbert Michel, Boraston Alisdair B

机构信息

Department of Biochemistry and Microbiology, University of Victoria, Victoria, BC V8W 3P6, Canada.

Human Health Therapeutics, National Research Council Canada, Ottawa, ON K1A 0R6, Canada.

出版信息

Proc Natl Acad Sci U S A. 2017 Jan 31;114(5):E679-E688. doi: 10.1073/pnas.1615141114. Epub 2017 Jan 17.

Abstract

The vast majority of proteins are posttranslationally altered, with the addition of covalently linked sugars (glycosylation) being one of the most abundant modifications. However, despite the hydrolysis of protein peptide bonds by peptidases being a process essential to all life on Earth, the fundamental details of how peptidases accommodate posttranslational modifications, including glycosylation, has not been addressed. Through biochemical analyses and X-ray crystallographic structures we show that to hydrolyze their substrates, three structurally related metallopeptidases require the specific recognition of O-linked glycan modifications via carbohydrate-specific subsites immediately adjacent to their peptidase catalytic machinery. The three peptidases showed selectivity for different glycans, revealing protein-specific adaptations to particular glycan modifications, yet always cleaved the peptide bond immediately preceding the glycosylated residue. This insight builds upon the paradigm of how peptidases recognize substrates and provides a molecular understanding of glycoprotein degradation.

摘要

绝大多数蛋白质在翻译后会发生改变,共价连接糖类(糖基化)是其中最常见的修饰之一。然而,尽管肽酶水解蛋白质肽键是地球上所有生命都必需的过程,但肽酶如何适应包括糖基化在内的翻译后修饰的基本细节尚未得到解决。通过生化分析和X射线晶体学结构,我们表明,为了水解其底物,三种结构相关的金属肽酶需要通过紧邻其肽酶催化机制的碳水化合物特异性亚位点对O-连接聚糖修饰进行特异性识别。这三种肽酶对不同的聚糖表现出选择性,揭示了蛋白质对特定聚糖修饰的特异性适应,但总是切割糖基化残基之前的肽键。这一见解建立在肽酶如何识别底物的范式基础上,并提供了对糖蛋白降解的分子理解。

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