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Sensitive and Structure-Informative N-Glycosylation Analysis by MALDI-MS; Ionization Fragmentation and Derivatization

机译:通过MALDI-MS进行灵敏且结构丰富的N-糖基化分析;电离碎片化和衍生化

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摘要

Mass spectrometry (MS) has become an indispensable tool for analyzing post translational modifications of proteins, including N-glycosylated molecules. Because most glycosylation sites carry a multitude of glycans, referred to as “glycoforms,” the purpose of an N-glycosylation analysis is glycoform profiling and glycosylation site mapping. Matrix-assisted laser desorption/ionization mass spectrometry (MALDI-MS) has unique characteristics that are suited for the sensitive analysis of N-glycosylated products. However, the analysis is often hampered by the inherent physico-chemical properties of N-glycans. Glycans are highly hydrophilic in nature, and therefore tend to show low ion yields in both positive- and negative-ion modes. The labile nature and complicated branched structures involving various linkage isomers make structural characterization difficult. This review focuses on MALDI-MS-based approaches for enhancing analytical performance in N-glycosylation research. In particular, the following three topics are emphasized: (1) Labeling for enhancing the ion yields of glycans and glycopeptides, (2) Negative-ion fragmentation for less ambiguous elucidation of the branched structure of N-glycans, (3) Derivatization for the stabilization and linkage isomer discrimination of sialic acid residues.
机译:质谱(MS)已成为分析蛋白质(包括N-糖基化分子)的翻译后修饰所必不可少的工具。由于大多数糖基化位点都带有称为“糖基”的多种聚糖,因此N-糖基化分析的目的是糖基图谱分析和糖基化位点作图。基质辅助激光解吸/电离质谱(MALDI-MS)具有独特的特性,适用于N-糖基化产物的灵敏分析。但是,分析通常会受到N-聚糖固有的物理化学性质的阻碍。聚糖本质上是高度亲水的,因此倾向于在​​正离子和负离子模式下均显示出较低的离子产率。不稳定的性质和涉及各种键合异构体的复杂分支结构使结构表征困难。这篇综述着重于基于MALDI-MS的方法来增强N-糖基化研究的分析性能。尤其要强调以下三个主题:(1)标记以提高聚糖和糖肽的离子产量;(2)负离子断裂,以较少歧义地阐明N-聚糖的支链结构;(3)衍生化唾液酸残基的稳定和连接异构体区分。

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