N-glycopeptide Signatures of IgA in Serum from Patients with Hepatitis B Virus-related Liver Diseases

Overview

Journal Mol Cell Proteomics

Specialties Biochemistry
Cell Biology
Molecular Biology

Date 2019 Sep 11

PMID 31501225

Citations 16

Authors

Shu Zhang

Xinyi Cao

Chao Liu

Wei Li

Wenfeng Zeng

Baiwen Li

Hao Chi

Mingqi Liu

Xue Qin

Lingyi Tang

Guoquan Yan

Zefan Ge

Yinkun Liu

Qiang Gao

Haojie Lu

Affiliations

Soon will be listed here.

Abstract

N-glycosylation alteration has been reported in liver diseases. Characterizing N-glycopeptides that correspond to N-glycan structure with specific site information enables better understanding of the molecular pathogenesis of liver damage and cancer. Here, unbiased quantification of N-glycopeptides of a cluster of serum glycoproteins with 40-55 kDa molecular weight (40-kDa band) was investigated in hepatitis B virus (HBV)-related liver diseases. We used an N-glycopeptide method based on O/O C-terminal labeling to obtain 82 comparisons of serum from patients with HBV-related hepatocellular carcinoma (HCC) and liver cirrhosis (LC). Then, multiple reaction monitoring (MRM) was performed to quantify N-glycopeptide relative to the protein content, especially in the healthy donor-HBV-LC-HCC cascade. TPLTAITK (H5N5S1F1) and (H5N4S2F1) corresponding to the glycopeptides of IgA were significantly elevated in serum from patients with HBV infection and even higher in HBV-related LC patients, as compared with healthy donor. In contrast, the two glycopeptides of IgA fell back down in HBV-related HCC patients. In addition, the variation in the abundance of two glycopeptides was not caused by its protein concentration. The altered N-glycopeptides might be part of a unique glycan signature indicating an IgA-mediated mechanism and providing potential diagnostic clues in HBV-related liver diseases.

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