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免疫进化:无风险则无发展。

Evolution of immunity: no development without risk.

机构信息

SignaBlok, Inc., P.O. Box 4064, Shrewsbury, MA, 01545, USA.

出版信息

Immunol Res. 2012 Jun;52(3):176-81. doi: 10.1007/s12026-011-8256-4.

Abstract

Signal transduction by cell surface receptors in the context of heterogeneous and variable cellular environments plays a pivotal role in regulating many biological processes, including development, activation, and homeostasis of the immune system. In some receptors, extracellular ligand-binding and intracellular signaling domains are located on the same protein chain (single-chain receptors), while in the so-called multichain immune recognition receptors (MIRRs), recognition and signaling functions are separated between different protein chains. Why did nature separate recognition and signaling functions for MIRRs, thereby increasing the risk of malfunction and potential attack by pathogens? The risk is real: in order to escape the immune response, viruses are able to disrupt functional coupling between recognition and signaling aspects of MIRR machinery. Intrinsic disorder of intracellular signal-generating regions of MIRRs adds further intrigue to the story. Why did nature select protein disorder for MIRRs to translate recognition of distinct antigens into appropriate activation signals that would induce specific functional outcomes? Here, I suggest that nature takes the risks associated with intrareceptor separation of functions as well as with the chaos and indeterminacy of protein disorder in exchange for providing diversity and variability of signal transduction. Not only does this phenomenon serve as the molecular basis for the development and evolution of the immune and other complex biological systems, but it fits closely to Darwinian evolutionary biology.

摘要

细胞表面受体在异质和多变的细胞环境中进行信号转导,在调节许多生物学过程中起着关键作用,包括免疫系统的发育、激活和稳态。在一些受体中,细胞外配体结合和细胞内信号转导结构域位于同一蛋白链上(单链受体),而在所谓的多链免疫识别受体(MIRRs)中,识别和信号转导功能分别位于不同的蛋白链上。为什么自然界会将 MIRRs 的识别和信号转导功能分开,从而增加了受体功能失调和潜在病原体攻击的风险?这种风险是真实存在的:为了逃避免疫反应,病毒能够破坏 MIRR 机械中识别和信号转导方面的功能偶联。MIRRs 细胞内信号生成区域的固有无序性为这个故事增添了更多的复杂性。为什么自然界选择蛋白质无序来将不同抗原的识别转化为适当的激活信号,从而诱导特定的功能结果?在这里,我认为自然界承担了受体内部功能分离以及蛋白质无序的混沌和不确定性带来的风险,以换取信号转导的多样性和可变性。这种现象不仅是免疫和其他复杂生物系统发育和进化的分子基础,而且与达尔文进化生物学紧密契合。

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