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细胞受体胞质信号域中蛋白质内在无序的差异出现情况。

Differential occurrence of protein intrinsic disorder in the cytoplasmic signaling domains of cell receptors.

作者信息

Sigalov Alexander B, Uversky Vladimir N

机构信息

SignaBlok Inc.; Shrewsbury, MA USA.

出版信息

Self Nonself. 2011 Jan;2(1):55-72. doi: 10.4161/self.2.1.14790. Epub 2011 Jan 1.

Abstract

In human membrane proteins, intrinsically disordered regions, the regions that lack a well-defined three-dimensional structure under physiological conditions, preferentially occur in the cytoplasmic tails. Many of these proteins represent cell receptors that function by recognizing their cognate ligand outside the cell and translating this binding information into an intracellular activation signal. Based on location of recognition and signaling (effector) domains, functionally diverse and unrelated cell receptors can be classified into two main families: those in which binding and signaling domains are located on the same protein chain, the so-called single-chain receptors (SRs), and those in which these domains are intriguingly located on separate subunits, the so-called multichain receptors (MRs). Recognition domains of both SRs and MRs are known to be well ordered. In contrast, while cytoplasmic signaling domains of SRs are well-structured as well, those of MRs are intrinsically disordered. Despite important role of receptor signaling in health and disease, extensive comparative structural analysis of receptor signaling domains has not been carried out as of yet. In this study, using a variety of prediction algorithms, we show that protein disorder is a characteristic and distinctive feature of receptors with recognition and signaling functions distributed between separate protein chains. We also reveal that disorder distribution patterns are rather similar within SR subclasses suggesting potential functional explanations. Why did nature select protein disorder to provide intracellular signaling for MRs? Is there any correlation between disorder profiles of signaling domains and receptor function? These and other questions are addressed in this article.

摘要

在人类膜蛋白中,内在无序区域,即在生理条件下缺乏明确三维结构的区域,优先出现在细胞质尾部。这些蛋白中有许多代表细胞受体,其功能是识别细胞外的同源配体,并将这种结合信息转化为细胞内激活信号。根据识别域和信号(效应)域的位置,功能多样且不相关的细胞受体可分为两个主要家族:那些结合域和信号域位于同一蛋白链上的受体,即所谓的单链受体(SRs),以及那些这些域有趣地位于不同亚基上的受体,即所谓的多链受体(MRs)。已知SRs和MRs的识别域都是有序的。相比之下,虽然SRs的细胞质信号域结构也很良好,但MRs的细胞质信号域是内在无序的。尽管受体信号在健康和疾病中起着重要作用,但截至目前尚未对受体信号域进行广泛的比较结构分析。在本研究中,我们使用多种预测算法表明,蛋白质无序是识别和信号功能分布在不同蛋白链上的受体的一个特征性和独特特征。我们还揭示,无序分布模式在SR亚类中相当相似,这暗示了潜在的功能解释。为什么自然界选择蛋白质无序来为MRs提供细胞内信号传导?信号域的无序特征与受体功能之间是否存在任何关联?本文将探讨这些及其他问题。

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