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Optimized Fragmentation for Quantitative Analysis of Fucosylated N-Glycoproteins by LC-MS-MRM

机译:LC-MS-MRM用岩藻糖苷化的N-糖蛋白的定量分析优化的碎片

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摘要

Quantitative analysis of site specific glycoforms of proteins is technically challenging but highly desirable; resolution of the fucosylated glycoforms is of particular interest due to their biological importance. In this study, we developed a sensitive and specific LC-MS-MRM quantification method that distinguishes the outer arm and core fucosylated configurations of the N-glycopeptides. We take advantage of limited fragmentation of the glycopeptides at low collision energy CID to produce linkage-specific Y-ions. We select these informative ions as MRM transitions for the quantification of the outer arm and total fucosylation of 12 fucosylated glycoforms of 9 glycopeptides in 7 plasma proteins. Our workflow showed improved sensitivity and specificity of quantification of the glycopeptides compared to oxonium ion transitions which allowed us to quantify the glycoforms directly in plasma or serum without fractionation of the samples or glycopeptide enrichment. A pilot study of fucosylation in liver cirrhosis of the HCV and NASH etiologies confirms the quantitative capabilities of the method and shows that liver cirrhosis is consistently associated with increased outer arm fucosylation of majority of the analyzed proteins. The results show that the outer arm fucosylation of the A2G2F1 glycoform of the VDKDLQSLEDILHQVENK peptide of fibrinogen increases greater than 10-fold in the HCV and NASH patients compared to healthy controls.
机译:蛋白质特异性糖族的定量分析技术上挑战,但非常需要;由于它们的生物重要性,岩氧化糖族的分辨率特别感兴趣。在这项研究中,我们开发了一种敏感和特异性的LC-MS-MRM定量方法,其区分N-糖肽的外臂和核心岩藻糖基化构型。我们利用低碰撞能量CID在低碰撞能量CID下有限的糖肽的碎片化,以产生胶合特异性的Y型离子。我们选择这些信息离子作为MRM过渡,以定量在7个血浆蛋白中为9糖肽的12个岩氧化糖糖苷的外臂和总岩岩化。与氧铵离子转变相比,我们的工作流程显示出改善的糖肽的定量敏感性和特异性,其使我们使我们能够直接在等离子体或血清中量化糖醇而不会分馏样品或糖肽富集。 HCV和NASH病因肝硬化中岩藻糖基化的试验研究证实了该方法的定量能力,并表明肝硬化与大多数分析蛋白质的外臂岩岩化始终如一。结果表明,与健康对照相比,纤维蛋白原纤维蛋白原的纤维蛋白原的A2G2F1甘油膜的外臂岩岩化纤维蛋白原的增加大于10倍。

著录项

  • 来源
    《Analytical chemistry》 |2019年第14期|共7页
  • 作者单位

    Georgetown Univ Lombardi Comprehens Canc Ctr Dept Oncol Washington DC 20057 USA;

    Georgetown Univ Lombardi Comprehens Canc Ctr Dept Oncol Washington DC 20057 USA;

    Georgetown Univ Lombardi Comprehens Canc Ctr Dept Oncol Washington DC 20057 USA;

    Georgetown Univ Lombardi Comprehens Canc Ctr Dept Oncol Washington DC 20057 USA;

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

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