Integrated <i>N</i>-glycoproteomics Analysis of Human Saliva for Lung Cancer

糖蛋白组学 唾液 糖蛋白 肺癌 癌症 聚糖 生物 粘蛋白 蛋白质组学 结合珠蛋白 糖基化 免疫学 医学 病理 内科学 分子生物学 生物化学 基因
作者
Sha Liu,Huiyu Wang,Xiaoteng Jiang,Yin Ji,Zeyuan Wang,Yan Zhang,Peng Wang,Hua Xiao
出处
期刊:Journal of Proteome Research [American Chemical Society]
标识
DOI:10.1021/acs.jproteome.1c00701
摘要

Aberrant protein N-glycosylation is a cancer hallmark, which has great potential for cancer detection. However, large-scale and in-depth analysis of N-glycosylation remains challenging because of its high heterogeneity, complexity, and low abundance. Human saliva is an attractive diagnostic body fluid, while few efforts explored its N-glycoproteome for lung cancer. Here, we utilized a zwitterionic-hydrophilic interaction chromatography-based strategy to specifically enrich salivary glycopeptides. Through quantitative proteomics analysis, 1492 and 1234 intact N-glycopeptides were confidently identified from pooled saliva samples of 10 subjects in the nonsmall-cell lung cancer group and 10 subjects in the normal control group. Accordingly, 575 and 404 N-glycosites were revealed for the lung cancer group and normal control group. In particular, 154 N-glycosites and 259 site-specific glycoforms were significantly dysregulated in the lung cancer group. Several N-glycosites located at the same glycoprotein and glycans attached to the same N-glycosites were observed with differential expressions, including haptoglobin, Mucin-5B, lactotransferrin, and α-1-acid glycoprotein 1. These N-glycoproteins were mainly related to inflammatory responses, infectious diseases, and cancers. Our study achieved comprehensive characterization of salivary N-glycoproteome, and dysregulated site-specific glycoforms hold promise for noninvasive detection of lung cancer.
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