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氢/氘交换质谱中的计算方法和挑战。

Computational methods and challenges in hydrogen/deuterium exchange mass spectrometry.

机构信息

I-BioStat, Hasselt University, Campus Diepenbeek, Agoralaan Gebouw D, Diepenbeek 3590, Belgium.

Statistics and Medical informatics Unit, Medical University of Bialystok, Białystok, Poland.

出版信息

Mass Spectrom Rev. 2017 Sep;36(5):649-667. doi: 10.1002/mas.21519. Epub 2016 Sep 7.

Abstract

Hydrogen/Deuterium exchange (HDX) has been applied, since the 1930s, as an analytical tool to study the structure and dynamics of (small) biomolecules. The popularity of using HDX to study proteins increased drastically in the last two decades due to the successful combination with mass spectrometry (MS). Together with this growth in popularity, several technological advances have been made, such as improved quenching and fragmentation. As a consequence of these experimental improvements and the increased use of protein-HDXMS, large amounts of complex data are generated, which require appropriate analysis. Computational analysis of HDXMS requires several steps. A typical workflow for proteins consists of identification of (non-)deuterated peptides or fragments of the protein under study (local analysis), or identification of the deuterated protein as a whole (global analysis); determination of the deuteration level; estimation of the protection extent or exchange rates of the labile backbone amide hydrogen atoms; and a statistically sound interpretation of the estimated protection extent or exchange rates. Several algorithms, specifically designed for HDX analysis, have been proposed. They range from procedures that focus on one specific step in the analysis of HDX data to complete HDX workflow analysis tools. In this review, we provide an overview of the computational methods and discuss outstanding challenges. © 2016 Wiley Periodicals, Inc. Mass Spec Rev 36:649-667, 2017.

摘要

氢/氘交换(HDX)自 20 世纪 30 年代以来一直被用作研究(小)生物分子结构和动态的分析工具。由于与质谱(MS)的成功结合,过去二十年中使用 HDX 研究蛋白质的应用越来越广泛。随着这种普及程度的提高,已经取得了一些技术进步,例如改进的淬灭和碎裂。由于这些实验改进和蛋白质-HDXMS 的增加使用,产生了大量复杂的数据,需要进行适当的分析。HDXMS 的计算分析需要几个步骤。蛋白质的典型工作流程包括鉴定(非)氘化肽或研究中蛋白质的片段(局部分析),或鉴定整个氘化蛋白质(全局分析);确定氘化水平;估计易变的骨干酰胺氢原子的保护程度或交换速率;以及对估计的保护程度或交换速率进行统计学上合理的解释。已经提出了几种专门用于 HDX 分析的算法。它们的范围从专注于 HDX 数据分析中一个特定步骤的程序到完整的 HDX 工作流程分析工具。在这篇综述中,我们提供了计算方法的概述,并讨论了尚未解决的挑战。 © 2016 Wiley Periodicals, Inc. Mass Spec Rev 36:649-667, 2017.

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