H/D 交换中心监测不足以显示蛋白质状态行为的差异。
H/D exchange centroid monitoring is insufficient to show differences in the behavior of protein states.
机构信息
Department of Chemistry, Washington University in St. Louis, St. Louis, MO 63130, USA.
出版信息
J Am Soc Mass Spectrom. 2013 Mar;24(3):450-3. doi: 10.1007/s13361-012-0555-z. Epub 2013 Feb 9.
Abstract
Differential hydrogen/deuterium exchange (H/DX) coupled with mass spectrometry (H/DX-MS) offers a rapid and sensitive characterization of changes in proteins following perturbations induced by changes in folding, ligand binding, oligomerization, and modification. The characterization of H/DX rates by software tools and automated data processing often relies on the centroid mass calculation and, thereby, the deuterium distribution in the mass spectra is neglected. Here we present an example demonstrating the clear limitation of using only a centroid approach to characterize the H/DX rate, in which the change in protein is not reflected as the difference in deuterium uptake based on centroid calculation.
摘要
差分式氢/氘交换(H/DX)结合质谱(H/DX-MS)为研究折叠、配体结合、寡聚化和修饰等因素引起的蛋白质构象变化提供了一种快速而灵敏的蛋白质结构变化特征分析方法。通过软件工具和自动化数据处理对 H/DX 速率进行特征分析时,通常依赖于质心质量计算,从而忽略了质谱中氘的分布。本文通过一个实例演示了仅使用质心方法来对 H/DX 速率进行特征分析的明显局限性,在这种方法中,基于质心计算的氘摄入差异无法反映蛋白质的变化。
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