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Navigating membrane protein structure dynamics and energy landscapes using spin labeling and EPR spectroscopy

机译:使用自旋标记和EPR光谱导航膜蛋白结构动力学和能量分布

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摘要

A detailed understanding of the functional mechanism of a protein entails the characterization of its energy landscape. Achieving this ambitious goal requires the integration of multiple approaches including determination of high resolution crystal structures, uncovering conformational sampling under distinct biochemical conditions, characterizing the kinetics and thermodynamics of transitions between functional intermediates using spectroscopic techniques, and interpreting and harmonizing the data into novel computational models. With increasing sophistication in solution-based and ensemble-oriented biophysical approaches such as electron paramagnetic resonance (EPR) spectroscopy, atomic resolution structural information can be directly linked to conformational sampling in solution. Here, we detail how recent methodological and technological advances in EPR spectroscopy have contributed to the elucidation of membrane protein mechanisms. Furthermore, we aim to assist investigators interested in pursuing EPR studies by providing an introduction to the technique, a primer on experimental design, and a description of the practical considerations of the method towards generating high quality data.
机译:对蛋白质功能机制的详细了解需要对其能量格局进行表征。要实现这一宏伟目标,就需要整合多种方法,包括确定高分辨率的晶体结构,在不同的生化条件下揭示构象采样,使用光谱技术表征功能中间体之间的跃迁动力学和热力学以及将数据解释和协调为新颖的计算模型。 。随着基于溶液和面向集合的生物物理方法(如电子顺磁共振(EPR)光谱学)的复杂性不断提高,原子分辨率的结构信息可以直接与溶液中的构象采样联系起来。在这里,我们详细介绍了EPR光谱学的最新方法学和技术进步如何有助于阐明膜蛋白机制。此外,我们旨在通过介绍该技术,实验设计入门以及对生成高质量数据的方法的实际考虑的描述,来协助有兴趣进行EPR研究的研究人员。

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