Cooperativity in biological systems

R. Behrouzi
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Abstract

Living organisms can sense and respond to external and internal stimuli. Response isdemonstrated in many forms including modulation of gene expression profiles, motility,secretion, cell death, etc. Nevertheless, all forms share a basic property: they depend on sensingsmall changes in the concentration of an effector molecule or subtle conformational changes ina protein and invoking the appropriate molecular response by the relevant signaling pathways.Sensing, transduction, and response to signals may be directly carried out by controlled changesin the conformation or the assembly of pre-existing components(1,2)or may involve changes ingene expression patterns (as in cell differentiation and development), which in turn is carriedout by protein-nucleic acid interactions and complex formation. Hence, understandingconformational changes in proteins and nucleic acids, ligand binding, and complex formationplay acentral role in advancing our knowledge of cellular dynamics. Large-scale interactionmapping projects continue to provide detailed (though approximate) interaction networksbetween pairs of proteins (3–6), but fall short of capturing the stability or dynamics of theinteractions. Integration of these maps with thermodynamic and kinetic information aboutconformational changes and binding events in proteins and nucleic acids holds the promise ofdiscovering simple universal mechanisms that explain and relate seemingly disparate biologicalphenomena at many levels of complexity. In this article, I will explore ‘cooperativity’, one ofthe most ubiquitous features in molecular biology and discuss how it impacts macromolecularfolding, complex assembly, formation of biological networks, and eventually cellular functionand pathology.
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生物系统中的协同性
生物体能够感知外部和内部刺激并作出反应。反应表现为多种形式,包括基因表达谱的调节、运动、分泌、细胞死亡等。然而,所有形式都有一个基本特性:它们依赖于感知效应分子浓度的微小变化或蛋白质中细微的构象变化,并通过相关的信号通路调用适当的分子反应。信号的感知、转导和响应可以直接通过控制构象的变化或预先存在的成分的组装来完成(1,2),或者可能涉及基因表达模式的变化(如在细胞分化和发育中),而基因表达模式的变化反过来又通过蛋白质-核酸相互作用和复合物的形成来完成。因此,了解蛋白质和核酸的构象变化、配体结合和复合物的形成在提高我们对细胞动力学的认识方面发挥着核心作用。大规模的相互作用映射项目继续提供蛋白质对之间的详细(尽管是近似的)相互作用网络(3-6),但缺乏捕获相互作用的稳定性或动态。将这些图谱与蛋白质和核酸的构象变化和结合事件的热力学和动力学信息相结合,有望发现简单的通用机制,这些机制可以解释和联系许多复杂程度上看似不同的生物现象。在这篇文章中,我将探讨“协同性”,这是分子生物学中最普遍的特征之一,并讨论它如何影响大分子折叠、复杂组装、生物网络的形成,以及最终的细胞功能和病理。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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