Radiolytic protein footprinting with mass spectrometry to probe the structure of macromolecular complexes.

Keiji Takamoto, Mark R Chance
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引用次数: 233

Abstract

Structural proteomics approaches using mass spectrometry are increasingly used in biology to examine the composition and structure of macromolecules. Hydroxyl radical-mediated protein footprinting using mass spectrometry has recently been developed to define structure, assembly, and conformational changes of macromolecules in solution based on measurements of reactivity of amino acid side chain groups with covalent modification reagents. Accurate measurements of side chain reactivity are achieved using quantitative liquid-chromatography-coupled mass spectrometry, whereas the side chain modification sites are identified using tandem mass spectrometry. In addition, the use of footprinting data in conjunction with computational modeling approaches is a powerful new method for testing and refining structural models of macromolecules and their complexes. In this review, we discuss the basic chemistry of hydroxyl radical reactions with peptides and proteins, highlight various approaches to map protein structure using radical oxidation methods, and describe state-of-the-art approaches to combine computational and footprinting data.

用质谱法探测大分子复合物结构的辐射分解蛋白足迹。
结构蛋白质组学方法使用质谱法在生物学中越来越多地用于检查大分子的组成和结构。最近,羟基自由基介导的蛋白质足迹利用质谱技术被开发出来,通过测量氨基酸侧链基团与共价修饰试剂的反应性来定义溶液中大分子的结构、组装和构象变化。侧链反应性的精确测量是使用定量液相色谱耦合质谱法实现的,而侧链修饰位点是使用串联质谱法确定的。此外,利用足迹数据与计算建模方法相结合,是测试和完善大分子及其复合物结构模型的一种强大的新方法。在这篇综述中,我们讨论了羟基自由基与肽和蛋白质反应的基本化学,重点介绍了使用自由基氧化方法绘制蛋白质结构的各种方法,并描述了将计算和足迹数据相结合的最新方法。
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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