ADP-ribosylserine hydrolase ARH3 of Latimeria chalumnae in complex with ADP-ribosyl-L-arginine

Chemistry & biology Pub Date : 2018-11-28 DOI:10.2210/PDB6HH4/PDB

J. Rack, Antonio Ayala Ariza, Bryon S. Drown, Callum Henfrey, Edward J. Bartlett, T. Shirai, P. Hergenrother, I. Ahel

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引用次数: 1

Abstract

Summary Protein ADP-ribosylation is a highly dynamic post-translational modification. The rapid turnover is achieved, among others, by ADP-(ribosyl)hydrolases (ARHs), an ancient family of enzymes that reverses this modification. Recently ARHs came into focus due to their role as regulators of cellular stresses and tumor suppressors. Here we present a comprehensive structural analysis of the enzymatically active family members ARH1 and ARH3. These two enzymes have very distinct substrate requirements. Our data show that binding of the adenosine ribose moiety is highly diverged between the two enzymes, whereas the active sites harboring the distal ribose closely resemble each other. Despite this apparent similarity, we elucidate the structural basis for the selective inhibition of ARH3 by the ADP-ribose analogues ADP-HPD and arginine-ADP-ribose. Together, our biochemical and structural work provides important insights into the mode of enzyme-ligand interaction, helps to understand differences in their catalytic behavior, and provides useful tools for targeted drug design.

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与adp -核糖基- l-精氨酸配合物的紫堇adp -核糖基丝氨酸水解酶ARH3

蛋白质adp核糖基化是一种高度动态的翻译后修饰。ADP-(核糖基)水解酶(ARHs)是一种古老的酶家族，可以逆转这种修饰。近年来，ARHs因其作为细胞应激调节因子和肿瘤抑制因子的作用而成为关注的焦点。在此，我们对酶活性家族成员ARH1和ARH3进行了全面的结构分析。这两种酶对底物的要求非常不同。我们的数据表明，两种酶之间的腺苷核糖片段的结合高度分化，而远端核糖的活性位点彼此非常相似。尽管这种明显的相似性，我们阐明了adp -核糖类似物ADP-HPD和精氨酸- adp -核糖选择性抑制ARH3的结构基础。总之，我们的生化和结构工作提供了对酶-配体相互作用模式的重要见解，有助于理解它们的催化行为差异，并为靶向药物设计提供有用的工具。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Chemistry & biology 生物-生化与分子生物学

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审稿时长

4-8 weeks