Robust Glycoproteomics Platform Reveals a Tetra‐Antennary Site‐Specific Glycan Capping with Sialyl‐Lewis Antigen for Early Detection of Gastric Cancer

Author:

Liu Luyao12ORCID,Liu Lei12,Wang Yan1,Fang Zheng1,Bian Yangyang3,Zhang Wenyao4,Wang Zhongyu1,Gao Xianchun4,Zhao Changrui5,Tian Miaomiao4,Liu Xiaoyan1,Qin Hongqiang1,Guo Zhimou1,Liang Xinmiao1,Dong Mingming5,Nie Yongzhan4,Ye Mingliang126ORCID

Affiliation:

1. CAS Key Laboratory of Separation Science for Analytical Chemistry, Dalian Institute of Chemical Physics Chinese Academy of Sciences Dalian 116023 China

2. University of Chinese Academy of Sciences Beijing 101408 China

3. The College of Life Sciences Northwest University Xi'an 710127 China

4. State Key Laboratory of Cancer Biology, Xijing Hospital of Digestive Diseases Fourth Military Medical University Xi'an 710068 China

5. MOE Key Laboratory of Bio‐Intelligent Manufacturing, School of Bioengineering Dalian University of Technology Dalian 116024 China

6. State Key Laboratory of Medical Proteomics Beijing 102206 China

Abstract

AbstractThe lack of efficient biomarkers for the early detection of gastric cancer (GC) contributes to its high mortality rate, so it is crucial to discover novel diagnostic targets for GC. Recent studies have implicated the potential of site‐specific glycans in cancer diagnosis, yet it is challenging to perform highly reproducible and sensitive glycoproteomics analysis on large cohorts of samples. Here, a highly robust N‐glycoproteomics (HRN) platform comprising an automated enrichment method, a stable microflow LC‐MS/MS system, and a sensitive glycopeptide‐spectra‐deciphering tool is developed for large‐scale quantitative N‐glycoproteome analysis. The HRN platform is applied to analyze serum N‐glycoproteomes of 278 subjects from three cohorts to investigate glycosylation changes of GC. It identifies over 20 000 unique site‐specific glycans from discovery and validation cohorts, and determines four site‐specific glycans as biomarker candidates. One candidate has branched tetra‐antennary structure capping with sialyl‐Lewis antigen, and it significantly outperforms serum CEA with AUC values > 0.89 compared against < 0.67 for diagnosing early‐stage GC. The four‐marker panel can provide improved diagnostic performances. Besides, discrimination powers of four candidates are also testified with a verification cohort using PRM strategy. This findings highlight the value of this strong tool in analyzing aberrant site‐specific glycans for cancer detection.

Funder

National Natural Science Foundation of China

Publisher

Wiley

Subject

General Physics and Astronomy,General Engineering,Biochemistry, Genetics and Molecular Biology (miscellaneous),General Materials Science,General Chemical Engineering,Medicine (miscellaneous)

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