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Recent Advances and Applications in Synchrotron X-Ray Protein Footprinting for Protein Structure and Dynamics Elucidation

机译:同步加速器X射线蛋白质足迹用于蛋白质结构和动力学阐明的最新进展和应用

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摘要

Synchrotron X-ray Footprinting is a powerful in situ hydroxyl radical labeling method for analysis of protein structure, interactions, folding and conformation change in solution. In this method, water is ionized by high flux density broad band synchrotron X-rays to produce a steady-state concentration of hydroxyl radicals, which then react with solvent accessible side-chains. The resulting stable modification products are analyzed by liquid chromatography coupled to mass spectrometry. A comparative reactivity rate between known and unknown states of a protein provides local as well as global information on structural changes, which is then used to develop structural models for protein function and dynamics. In this review we describe the XF-MS method, its unique capabilities and its recent technical advances at the Advanced Light Source. We provide a comparison of other hydroxyl radical and mass spectrometry based methods with XF-MS. We also discuss some of the latest developments in its usage for studying bound water, transmembrane proteins and photosynthetic protein components, and the synergy of the method with other synchrotron based structural biology methods.
机译:Synchrotron X射线足迹法是一种强大的原位羟基自由基标记方法,可用于分析溶液中的蛋白质结构,相互作用,折叠和构象变化。在这种方法中,水被高通量密度宽带同步加速器X射线电离,产生稳态浓度的羟基自由基,然后与溶剂可及的侧链反应。通过液相色谱-质谱法分析所得的稳定的改性产物。蛋白质已知状态和未知状态之间的比较反应速率可提供有关结构变化的局部以及全局信息,然后将其用于开发蛋白质功能和动力学的结构模型。在本文中,我们将介绍XF-MS方法,其独特功能以及其在Advanced Light Source上的最新技术进步。我们提供了使用XF-MS对其他基于羟基自由基和质谱的方法的比较。我们还将讨论其在研究结合水,跨膜蛋白和光合蛋白成分方面的最新发展,以及该方法与其他基于同步加速器的结构生物学方法的协同作用。

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