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首页> 外文期刊>Analytical chemistry >Identification of Lewis and Blood Group Carbohydrate Epitopes by Ion Mobility-Tandem-Mass Spectrometry Fingerprinting
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Identification of Lewis and Blood Group Carbohydrate Epitopes by Ion Mobility-Tandem-Mass Spectrometry Fingerprinting

机译:离子迁移率 - 串联光谱法鉴定路易斯和血液碳水化合物表位

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摘要

Glycans have several elements that contribute to their structural complexity, involving a range of monosaccharide building blocks, configuration of linkages between residues and various degrees of branching on a given structure. Their analysis remains challenging and resolving minor isomeric variants can be difficult, in particular terminal fucosylated Lewis and blood group antigens present on Nand O-glycans. Accurately characterizing these isomeric structures by current techniques is not straightforward and typically requires a combination of methods and/or sample derivatization. Yet the ability to monitor the occurrence of these epitopes is important as structural changes are associated with several human diseases. The use of ion mobility-mass spectrometry (IM-MS), which separates ions in the gas phase based on their size, charge and shape, offers a new potential tool for glycan analysis and recent reports have demonstrated its potential for glycomics. Here we show that Lewis and blood group isomers, which have identical fragmentation spectra, exhibit very distinctive IM drift times and collision cross sections (CCS). We show that IM-MS/MS analysis can rapidly and accurately differentiate epitopes from parotid gland N-glycans and milk oligosaccharides based on fucosylated fragment ions with characteristic CCSs.
机译:聚糖具有若干元素,有助于其结构复杂性,涉及一系列单糖构造块,残留物之间的连杆和给定结构上的各种分支之间的配置。它们的分析仍然挑战性,并且可以难以解决较小的异构体变体,特别是末端岩氧化的lewis和存在于Nand O-聚糖上的血型抗原。通过电流技术精确地表征这些异构结构并不直接,并且通常需要方法和/或样品衍生化的组合。然而,监测这些表位的发生的能力是与结构变化与几种人类疾病有关的重要性。使用离子迁移率质谱(IM-MS),其基于其尺寸,电荷和形状将离子分离在气相中,为Glycan分析提供了新的潜在工具,并且最近的报告已经证明了其含量的含量。在这里,我们显示lewis和血型异构体具有相同的碎裂光谱,表现出非常独特的IM漂移时间和碰撞横截面(CCS)。我们表明IM-MS / MS分析可以快速准确地将来自腮腺N-聚糖的表位和基于具有特征CCSS的岩石化的片段离子的牛奶寡糖和牛奶寡糖分化。

著录项

  • 来源
    《Analytical chemistry》 |2017年第4期|共8页
  • 作者单位

    Max Planck Gesell Fritz Haber Inst Faradayweg 4-6 D-14195 Berlin Germany;

    Free Univ Berlin Inst Chem &

    Biochem Takustr 3 D-14195 Berlin Germany;

    Univ Oxford Dept Biochem Oxford Glycobiol Inst Oxford OX1 3QU England;

    Univ Oxford Dept Biochem Oxford Glycobiol Inst Oxford OX1 3QU England;

    Max Planck Gesell Fritz Haber Inst Faradayweg 4-6 D-14195 Berlin Germany;

    Univ Oxford Dept Biochem Oxford Glycobiol Inst Oxford OX1 3QU England;

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  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 分析化学;
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