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Glycan family analysis for deducing N-glycan topology from single MS

机译:糖家族分析可从单个MS推导N-聚糖拓扑

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摘要

Motivation: In the past few years, mass spectrometry (MS) has emerged as the premier tool for identification and quantification of biological molecules such as peptides and glycans. There are two basic strategies: single-MS, which uses a single round of mass analysis, and MS/MS (or higher order MSn), which adds one or more additional rounds of mass analysis, interspersed with fragmentation steps. Single-MS offers higher throughput, broader mass coverage and more direct quantitation, but generally much weaker identification. Single-MS, however, does work fairly well for the case of N-glycan identification, which are more constrained than other biological polymers. We previously demonstrated single-MS identification of N-glycans to the level of ‘cartoons’ (monosaccharide composition and topology) by a system that incorporates an expert's detailed knowledge of the biological sample. In this article, we explore the possibility of ab initio single-MS N-glycan identification, with the goal of extending single-MS, or primarily-single-MS, identification to non-expert users, novel conditions and unstudied tissues.
机译:动机:在过去的几年中,质谱(MS)成为鉴定和定量生物分子(如肽和聚糖)的主要工具。有两种基本策略:使用单轮质量分析的Single-MS,和使用片段化步骤穿插的MS / MS(或更高阶MSn)添加一轮或多轮其他质量分析。单质谱仪可提供更高的通量,更广泛的质量覆盖范围和更直接的定量分析,但通常鉴定要弱得多。但是,对于比其他生物聚合物更受约束的N-聚糖鉴定,Single-MS确实能很好地工作。之前,我们通过结合专家对生物样品的详细了解的系统,证明了将MS鉴定为“卡通”(单糖成分和拓扑结构)水平的N-聚糖的能力。在本文中,我们探索了从头开始进行单MS N-聚糖鉴定的可能性,其目标是将单MS或主要是单MS的鉴定扩展到非专家用户,新病况和未经研究的组织。

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