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Sulfate migration in oligosaccharides induced by negative ion mode ion trap collision-induced dissociation.寡糖在负离子模式离子阱碰撞诱导解离中诱导的硫酸盐迁移。
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Isomer-specific chromatographic profiling yields highly sensitive and specific potential N-glycan biomarkers for epithelial ovarian cancer.对映异构体特异性色谱分析可产生高度敏感和特异的上皮性卵巢癌潜在 N-糖链生物标志物。
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Attachment of chloride anion to sugars: mechanistic investigation and discovery of a new dopant for efficient sugar ionization/detection in mass spectrometers.氯离子与糖的结合:在质谱仪中有效实现糖离子化/检测的新型掺杂剂的机理研究与发现。
Chemistry. 2012 Oct 8;18(41):13059-67. doi: 10.1002/chem.201103788. Epub 2012 Aug 31.
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Production platforms for biotherapeutic glycoproteins. Occurrence, impact, and challenges of non-human sialylation.生物治疗性糖蛋白的生产平台。非人类唾液酸化的发生、影响和挑战。
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Ultrasensitive capillary electrophoretic analysis of potentially immunogenic carbohydrate residues in biologics: galactose-α-1,3-galactose containing oligosaccharides.超敏毛细管电泳分析生物技术中潜在免疫原性的碳水化合物残基:含有半乳糖-α-1,3-半乳糖的寡糖。
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Effective use of mass spectrometry for glycan and glycopeptide structural analysis.高效利用质谱技术进行聚糖和糖肽结构分析。
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Analysis of the acidic proteome with negative electron-transfer dissociation mass spectrometry.采用负离子电喷雾解析质谱法分析酸性蛋白质组。
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Annotation of a serum N-glycan library for rapid identification of structures.血清 N-聚糖文库的注释用于快速鉴定结构。
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Comprehensive native glycan profiling with isomer separation and quantitation for the discovery of cancer biomarkers.实现异构体分离和定量的综合天然聚糖分析,用于癌症生物标志物的发现。
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采用氟化物介导的负离子微流控芯片 LC-MS 对 N-连接寡糖进行深入表征。

In-depth characterization of N-linked oligosaccharides using fluoride-mediated negative ion microfluidic chip LC-MS.

机构信息

Barnett Institute of Chemical and Biological Analysis and Department of Chemistry and Chemical Biology, Northeastern University, Boston, Massachusetts 02115, United States.

出版信息

Anal Chem. 2013 Mar 19;85(6):3127-35. doi: 10.1021/ac3031898. Epub 2013 Feb 27.

DOI:10.1021/ac3031898
PMID:23398125
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3604099/
Abstract

Characterization of N-glycans by liquid chromatography-positive electrospray ionization (ESI) tandem mass spectrometry (LC-MS/MS) using a microfluidic chip packed with porous graphitized carbon (PGC) represents a rapidly developing area in oligosaccharide analysis. Positive ion ESI-MS generates B/Y-type glycosidic fragment ions under collisional-induced dissociation (CID). Although these ions facilitate glycan sequencing, they provide little information on linkage and positional isomers. Isomer identification in these cases is by retention on the PGC stationary phase where the specific structural isomers can, in principle, be separated. In this paper, we broaden the applicability of the PGC microfluidic chip/MS platform by implementing fluoride-mediated negative ESI-MS. Ammonium fluoride, added to the mobile phase, aids in the formation of pseudomolecular oligosaccharide anions due to the ability of fluoride to abstract a proton from the glycan structure. The negative charge results in the generation of C-type glycosidic fragments, highly informative A-type cross-ring fragment ions, and additional gas-phase ion reaction products (e.g., D- and E-type ions), which, when combined, lead to in-depth oligosaccharide characterization, including linkage and positional isomers. Due to the separation of anomers by the PGC phase, comparison of oligosaccharides with an intact reducing terminus to their experimentally prepared corresponding alditols was performed, revealing a more sensitive MS and, especially, MS/MS analysis from the glycans with a free reducing end. Fluoride also ensured recovery of charged oligosaccharides from the PGC stationary phase. Application to the characterization of N-glycans released from polyclonal human and murine serum IgG is presented to demonstrate the effectiveness of the chip/negative ESI approach.

摘要

利用填充有多孔石墨化碳(PGC)的微流控芯片通过液相色谱 - 正电喷雾电离(ESI)串联质谱(LC-MS/MS)对 N-糖进行表征是寡糖分析中一个迅速发展的领域。正离子 ESI-MS 在碰撞诱导解离(CID)下产生 B/Y 型糖苷键片段离子。虽然这些离子有助于糖测序,但它们提供的关于键和位置异构体的信息很少。在这些情况下,通过在 PGC 固定相上保留来进行异构体鉴定,其中特定的结构异构体原则上可以分离。在本文中,我们通过实施氟化物介导的负 ESI-MS 来拓宽 PGC 微流控芯片/ MS 平台的适用性。向流动相中添加氟化铵,由于氟化物能够从聚糖结构中提取质子,因此有助于形成假分子寡糖阴离子。负电荷导致 C 型糖苷键片段、高度信息丰富的 A 型跨环片段离子和附加的气相离子反应产物(例如 D-和 E-型离子)的生成,这些产物结合在一起,导致深入的寡糖表征,包括键和位置异构体。由于 PGC 相分离了差向异构体,因此对具有完整还原末端的寡糖与其实验制备的相应醛糖醇进行了比较,结果表明游离还原末端的聚糖具有更灵敏的 MS 分析,尤其是 MS/MS 分析。氟化物还确保了带电荷的寡糖从 PGC 固定相上的回收。该芯片/负 ESI 方法的应用已应用于从多克隆人血清 IgG 和鼠血清 IgG 中释放的 N-糖的表征,以证明该方法的有效性。