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Rapid N-Glycan Profiling of Serum and Plasma by a Novel Slide-Based Imaging Mass Spectrometry Workflow

Calvin R.K. Blaschke, Alyson Black, Anand S. Mehta, Peggi M. Angel, Richard R. Drake

2020Journal of the American Society for Mass Spectrometry38 citationsDOIOpen Access PDF

Abstract

Changes in the levels and compositions of N-glycans released from serum and plasma glycoproteins have been assessed in many diseases across many large clinical sample cohorts. Assays used for N-glycan profiling in these fluids currently require multiple processing steps and have limited throughput, thus diminishing their potential for use as standard clinical diagnostic assays. A novel slide-based N-glycan profiling method was evaluated for sensitivity and reproducibility using a pooled serum standard. Serum was spotted on to an amine-reactive slide, delipidated and desalted with a series of washes, sprayed with peptide N-glycosidase F and matrix, and analyzed by MALDI-FTICR or MALDI-Q-TOF mass spectrometry. Routinely, over 75 N-glycan species can be detected from one microliter of serum in less than 6.5 h. Additionally, endoglycosidase F3 was applied to this workflow to identify core-fucosylated N-glycans and displayed the adaptability of this method for the determination of structural information. This method was applied to a small pooled serum set from either obese or nonobese patients that had breast cancer or a benign lesion. This study confirms the reproducibility, sensitivity, and adaptability of a novel method for N-glycan profiling of serum and plasma for potential application to clinical diagnostics.

Topics & Concepts

GlycanChemistryGlycomicsMass spectrometryChromatographyMatrix-assisted laser desorption/ionizationReproducibilityEndoglycosidaseGlycoproteinBiochemistryAdsorptionDesorptionOrganic chemistryGlycosylation and Glycoproteins ResearchAdvanced Proteomics Techniques and ApplicationsMass Spectrometry Techniques and Applications