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Isomer-Specific Monitoring of Sialylated N-Glycans Reveals Association of alpha 2,3-Linked Sialic Acid Epitope With Behcet's Disease

Authors
Seo, NariLee, HyunjunOh, Myung JinKim, Ga HyeonLee, Sang GilAhn, Joong KyongCha, Hoon-SukKim, Kyoung HeonKim, JaehanAn, Hyun Joo
Issue Date
23-11월-2021
Publisher
FRONTIERS MEDIA SA
Keywords
Behcet' s disease; biomarker; glycan isomer; quantitation; sialic acid epitope
Citation
FRONTIERS IN MOLECULAR BIOSCIENCES, v.8
Indexed
SCIE
SCOPUS
Journal Title
FRONTIERS IN MOLECULAR BIOSCIENCES
Volume
8
URI
https://scholar.korea.ac.kr/handle/2021.sw.korea/135698
DOI
10.3389/fmolb.2021.778851
ISSN
2296-889X
Abstract
Behcet's disease (BD) is an immune disease characterized by chronic and relapsing systemic vasculitis of unknown etiology, which can lead to blindness and even death. Despite continuous efforts to discover biomarkers for accurate and rapid diagnosis and optimal treatment of BD, there is still no signature marker with high sensitivity and high specificity. As the link between glycosylation and the immune system has been revealed, research on the immunological function of glycans is being actively conducted. In particular, sialic acids at the terminus of glycoconjugates are directly implicated in immune responses, cell-cell/pathogen interactions, and tumor progression. Therefore, changes in sialic acid epitope in the human body are spotlighted as a new indicator to monitor the onset and progression of immune diseases. Here, we performed global profiling of N-glycan compositions derived from the sera of 47 healthy donors and 47 BD patients using matrix-assisted laser desorption/ionization-time of flight mass spectrometry (MALDI-TOF MS) to preferentially determine BD target glycans. Then, three sialylated biantennary N-glycans were further subjected to the separation of linkage isomers and quantification using porous graphitized carbon-liquid chromatography (PGC-LC)/multiple reaction monitoring (MRM)-MS. We were able to successfully identify 11 isomers with sialic acid epitopes from the three glycan compositions consisting of Hex(5)HexNAc(4)NeuAc(1), Hex(5)HexNAc(4)Fuc(1)NeuAc(1), and Hex(5)HexNAc(4)NeuAc(2). Among them, three isomers almost completely distinguished BD from control with high sensitivity and specificity with an area under the curve (AUC) of 0.945, suggesting the potential as novel BD biomarkers. In particular, it was confirmed that alpha 2,3-sialic acid at the terminus of biantennary N-glycan was the epitope associated with BD. In this study, we present a novel approach to elucidating the association between BD and glycosylation by tracing isomeric structures containing sialic acid epitopes. Isomer-specific glycan profiling is suitable for analysis of large clinical cohorts and may facilitate the introduction of diagnostic assays for other immune diseases.
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