化学
聚糖
另一个
离子迁移光谱法
单糖
壳聚糖
立体化学
质谱法
有机化学
色谱法
生物化学
糖蛋白
甲壳素
壳聚糖
作者
Ahmed Ben Faleh,Stephan Warnke,Priyanka Bansal,Robert P. Pellegrinelli,Irina Dyukova,Thomas R. Rizzo
出处
期刊:Analytical Chemistry
[American Chemical Society]
日期:2022-07-07
卷期号:94 (28): 10101-10108
被引量:10
标识
DOI:10.1021/acs.analchem.2c01181
摘要
Glycan analysis has evolved considerably during the last decade. The advent of high-resolution ion-mobility spectrometry has enabled the separation of isomers with only the slightest of structural differences. However, the ability to separate such species raises the problem of identifying all the mobility-resolved peaks that are observed, especially when analytical standards are not available. In this work, we report an approach based on the combination of IMSn with cryogenic vibrational spectroscopy to identify N-glycan reducing-end anomers. By identifying the reducing-end α and β anomers of diacetyl-chitobiose, which is a disaccharide that forms part of the common core of all N-glycans, we are able to assign mobility peaks to reducing anomers of a selection of N-glycans of different sizes, starting from trisaccharides such as Man-1 up to glycans containing nine monosaccharide units, such as G2. By building an infrared fingerprint database of the identified N-glycans, our approach allows unambiguous identification of mobility peaks corresponding to reducing-end anomers and distinguishes them from positional isomers that might be present in a complex mixture.
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