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TIA-1 Self-Multimerization, Phase Separation, and Recruitment into Stress Granules Are Dynamically Regulated by Zn.TIA-1 的自多聚化、相分离和应激颗粒募集被 Zn 动态调节。
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Intrinsically disordered sequences enable modulation of protein phase separation through distributed tyrosine motifs.无序序列通过分散的酪氨酸基序来调节蛋白质相分离。
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人工蛋白质聚合物与内在无序蛋白质的融合

Convergence of Artificial Protein Polymers and Intrinsically Disordered Proteins.

作者信息

Dzuricky Michael, Roberts Stefan, Chilkoti Ashutosh

机构信息

Department of Biomedical Engineering , Duke University , Durham , North Carolina 27708-0281 , United States.

出版信息

Biochemistry. 2018 May 1;57(17):2405-2414. doi: 10.1021/acs.biochem.8b00056. Epub 2018 Apr 23.

DOI:10.1021/acs.biochem.8b00056
PMID:29683665
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC6311704/
Abstract

A flurry of research in recent years has revealed the molecular origins of many membraneless organelles to be the liquid phase separation of intrinsically disordered proteins (IDPs). Consequently, protein disorder has emerged as an important driver of intracellular compartmentalization by providing specialized microenvironments chemically distinct from the surrounding medium. Though the importance of protein disorder and its relationship to intracellular phase behavior are clear, a detailed understanding of how such phase behavior can be predicted and controlled remains elusive. While research in IDPs has largely focused on the implications of structural disorder on cellular function and disease, another field, that of artificial protein polymers, has focused on the de novo design of protein polymers with controllable material properties. A subset of these polymers, specifically those derived from structural proteins such as elastin and resilin, are also disordered sequences that undergo liquid-liquid phase separation. This phase separation has been used in a variety of biomedical applications, and researchers studying these polymers have developed methods to precisely characterize and tune their phase behavior. Despite their disparate origins, both fields are complementary as they study the phase behavior of intrinsically disordered polypeptides. This Perspective hopes to stimulate collaborative efforts by highlighting the similarities between these two fields and by providing examples of how such collaboration could be mutually beneficial.

摘要

近年来,一系列研究揭示了许多无膜细胞器的分子起源是内在无序蛋白质(IDP)的液相分离。因此,蛋白质无序通过提供与周围介质化学性质不同的特殊微环境,已成为细胞内区室化的重要驱动力。尽管蛋白质无序的重要性及其与细胞内相行为的关系很明确,但对如何预测和控制这种相行为的详细理解仍然难以捉摸。虽然对IDP的研究主要集中在结构无序对细胞功能和疾病的影响上,但另一个领域,即人工蛋白质聚合物领域,专注于具有可控材料特性的蛋白质聚合物的从头设计。这些聚合物的一个子集,特别是那些衍生自弹性蛋白和 resilin 等结构蛋白的聚合物,也是经历液-液相分离的无序序列。这种相分离已被用于各种生物医学应用中,研究这些聚合物的研究人员已经开发出精确表征和调节其相行为的方法。尽管它们的起源不同,但这两个领域是互补的,因为它们都研究内在无序多肽的相行为。这篇综述希望通过强调这两个领域之间的相似性,并提供这种合作如何互利的例子,来激发合作努力。