细胞通过受控混乱的蛋白质紊乱实现跨膜信号转导的多样化。

Alexander B Sigalov
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引用次数: 0

摘要

细胞表面受体的功能是在细胞膜上传递信号,从而导致各种生物反应。从结构上看,根据细胞外配体结合域和细胞内信号域是位于同一条蛋白链上(单链受体,SRs)还是位于不同的亚基上(多链受体,MRs),这些整合蛋白可分为两大类。由于大多数 MRs 都是免疫受体,因此它们通常都被称为多链免疫识别受体(MIRRs)。最近的研究发现,与 SRs 结构良好的信号结构域不同,MIRRs 的信号结构域是内在无序区,即在生理条件下缺乏明确三维结构的区域。为什么自然界要将 MIRR 的识别和信号功能分开?为什么大自然选择通过混乱的蛋白质无序区为 MIRR 提供高度特异性的信号?在跨膜信号转导过程中,什么机制可以控制这种混乱,从而提供免疫反应的特异性和多样性?在此,我总结了最近的研究发现,这些发现不仅可以揭示这些问题和其他问题,还能大大增加我们对受体信号转导的理解,而受体信号转导是一个基本过程,在健康和疾病中发挥着至关重要的作用。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Cells diversify transmembrane signaling through the controlled chaos of protein disorder.

Cell surface receptors function to transduce signals across the cell membrane leading to a variety of biologic responses. Structurally, these integral proteins can be classified into two main families, depending on whether extracellular ligand-binding and intracellular signaling domains are located on the same protein chain (single-chain receptors, SRs) or on separate subunits (multichain receptors, MRs). Since most MRs are immune receptors, they are all commonly referred to as multi-chain immune recognition receptors (MIRRs). Recent studies reveal that, in contrast to well-structured signaling domains of SRs, those of MIRRs represent intrinsically disordered regions, the regions that lack a well-defined three-dimensional structure under physiological conditions. Why did nature separate recognition and signaling functions of MIRRs? Why for MIRRs did nature select to provide highly specific signaling through the chaos of protein disorder? What mechanisms could control this chaos in the process of transmembrane signal transduction to provide the specificity and diversity of the immune response? Here, I summarize recent findings that may not only shed light on these and other questions but also add significantly to our understanding of receptor signaling, a fundamental process that plays a critical role in health and disease.

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