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分子伴侣调节因子家族成员多功能性的内在无序角度:BAGs中都有什么?

What's in the BAGs? Intrinsic disorder angle of the multifunctionality of the members of a family of chaperone regulators.

作者信息

Marzullo Liberato, Turco Maria C, Uversky Vladimir N

机构信息

Department of Medicine, Surgery and Dentistry Schola Medica Salernitana, University of Salerno, Baronissi, Italy.

Research and Development Division, BIOUNIVERSA s.r.l., Baronissi, Italy.

出版信息

J Cell Biochem. 2022 Jan;123(1):22-42. doi: 10.1002/jcb.30123. Epub 2021 Aug 2.

DOI:10.1002/jcb.30123
PMID:34339540
Abstract

In humans, the family of Bcl-2 associated athanogene (BAG) proteins includes six members characterized by exceptional multifunctionality and engagement in the pathogenesis of various diseases. All of them are capable of interacting with a multitude of often unrelated binding partners. Such binding promiscuity and related functional and pathological multifacetedness cannot be explained or understood within the frames of the classical "one protein-one structure-one function" model, which also fails to explain the presence of multiple isoforms generated for BAG proteins by alternative splicing or alternative translation initiation and their extensive posttranslational modifications. However, all these mysteries can be solved by taking into account the intrinsic disorder phenomenon. In fact, high binding promiscuity and potential to participate in a broad spectrum of interactions with multiple binding partners, as well as a capability to be multifunctional and multipathogenic, are some of the characteristic features of intrinsically disordered proteins and intrinsically disordered protein regions. Such functional proteins or protein regions lacking unique tertiary structures constitute a cornerstone of the protein structure-function continuum concept. The aim of this paper is to provide an overview of the functional roles of human BAG proteins from the perspective of protein intrinsic disorder which will provide a means for understanding their binding promiscuity, multifunctionality, and relation to the pathogenesis of various diseases.

摘要

在人类中,Bcl-2相关抗凋亡基因(BAG)蛋白家族包括六个成员,其特点是具有非凡的多功能性,并参与各种疾病的发病机制。它们都能够与众多通常不相关的结合伴侣相互作用。这种结合的混杂性以及相关的功能和病理多面性无法在经典的“一种蛋白质-一种结构-一种功能”模型框架内得到解释或理解,该模型也无法解释通过可变剪接或可变翻译起始为BAG蛋白产生的多种异构体的存在及其广泛的翻译后修饰。然而,考虑到内在无序现象,所有这些谜团都可以得到解决。事实上,高结合混杂性、参与与多个结合伴侣的广泛相互作用的潜力,以及多功能和多致病的能力,是内在无序蛋白质和内在无序蛋白质区域的一些特征。这种缺乏独特三级结构的功能性蛋白质或蛋白质区域构成了蛋白质结构-功能连续体概念的基石。本文的目的是从蛋白质内在无序的角度概述人类BAG蛋白的功能作用,这将为理解它们的结合混杂性、多功能性以及与各种疾病发病机制的关系提供一种方法。

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