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解析膜内蛋白酶菱形蛋白酶家族中的结构-功能关系。

Untangling structure-function relationships in the rhomboid family of intramembrane proteases.

作者信息

Brooks Cory L, Lemieux M Joanne

机构信息

Membrane Protein Disease Research Group, Department of Biochemistry, University of Alberta, Edmonton, Alberta, Canada, T6G 2H7.

出版信息

Biochim Biophys Acta. 2013 Dec;1828(12):2862-72. doi: 10.1016/j.bbamem.2013.05.003.

Abstract

Rhomboid proteases are a family of integral membrane proteins that have been implicated in critical regulatory roles in a wide array of cellular processes and signaling events. The determination of crystal structures of the prokaryotic rhomboid GlpG from Escherichia coli and Haemophilus influenzae has ushered in an era of unprecedented understanding into molecular aspects of intramembrane proteolysis by this fascinating class of protein. A combination of structural studies by X-ray crystallography, and biophysical and spectroscopic analyses, combined with traditional enzymatic and functional analysis has revealed fundamental aspects of rhomboid structure, substrate recognition and the catalytic mechanism. This review summarizes these remarkable advances by examining evidence for the proposed catalytic mechanism derived from inhibitor co-crystal structures, conflicting models of rhomboid-substrate interaction, and recent work on the structure and function of rhomboid cytosolic domains. In addition to exploring progress on aspects of rhomboid structure, areas for future research and unaddressed questions are emphasized and highlighted. This article is part of a Special Issue entitled: Intramembrane Proteases.

摘要

类菱形蛋白酶是一类整合膜蛋白家族,它们在众多细胞过程和信号事件中发挥关键的调节作用。对来自大肠杆菌和流感嗜血杆菌的原核类菱形蛋白酶GlpG晶体结构的测定,开启了一个对这类迷人蛋白质进行膜内蛋白水解分子层面前所未有的理解的时代。X射线晶体学的结构研究、生物物理和光谱分析,以及传统的酶学和功能分析相结合,揭示了类菱形蛋白酶结构、底物识别和催化机制的基本方面。本综述通过研究来自抑制剂共晶体结构的拟催化机制证据、类菱形蛋白酶-底物相互作用的矛盾模型以及类菱形蛋白酶胞质结构域结构和功能的最新研究成果,总结了这些显著进展。除了探讨类菱形蛋白酶结构方面的进展外,还强调并突出了未来研究的领域和未解决的问题。本文是名为“膜内蛋白酶”的特刊的一部分。

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