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Deconstructing thermodynamic parameters of a coupled system from site-specific observables

机译:从特定位置的观测值解构耦合系统的热力学参数

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摘要

Cooperative interactions mediate information transfer between structural domains of a protein molecule and are major determinants of protein function and modulation. The prevalent theories to understand the thermodynamic origins of cooperativity have been developed to reproduce the complex behavior of a global thermodynamic observable such as ligand binding or enzyme activity. However, in most cases the measurement of a single global observable cannot uniquely define all the terms that fully describe the energetics of the system. Here we establish a theoretical groundwork for analyzing protein thermodynamics using site-specific information. Our treatment involves extracting a site-specific parameter (defined as χ value) associated with a structural unit. We demonstrate that, under limiting conditions, the χ value is related to the direct interaction terms associated with the structural unit under observation and its intrinsic activation energy. We also introduce a site-specific interaction energy term (χdiff) that is a function of the direct interaction energy of that site with every other site in the system. When combined with site-directed mutagenesis and other molecular level perturbations, analyses of χ values of site-specific observables may provide valuable insights into protein thermodynamics and structure.
机译:合作相互作用介导了蛋白质分子结构域之间的信息传递,并且是蛋白质功能和调节的主要决定因素。已经开发了理解合作性热力学起源的流行理论,以再现可观察到的整体热力学的复杂行为,例如配体结合或酶活性。但是,在大多数情况下,对单个全局可观测值的度量无法唯一定义完全描述系统能量的所有术语。在这里,我们建立了使用特定位置信息分析蛋白质热力学的理论基础。我们的处理方法涉及提取与结构单元相关的特定位置参数(定义为χ值)。我们证明,在限制条件下,χ值与与观察中的结构单元及其固有活化能相关的直接相互作用项有关。我们还引入了特定于站点的相互作用能项(χ diff ),该项是该站点与系统中其他站点的直接交互能的函数。当与定点诱变和其他分子水平的扰动结合使用时,对定点可观察物的χ值的分析可能为蛋白质热力学和结构提供有价值的见解。

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