4.7 Article

Quantitative Longitudinal Inventory of the N-Glycoproteome of Human Milk from a Single Donor Reveals the Highly Variable Repertoire and Dynamic Site-Specific Changes

期刊

JOURNAL OF PROTEOME RESEARCH
卷 19, 期 5, 页码 1941-1952

出版社

AMER CHEMICAL SOC
DOI: 10.1021/acs.jproteome.9b00753

关键词

human milk; glycoprotein; milk proteins; glycopeptides; HILIC-based platform; mass spectrometry; N-glycosylation; N-glycopeptide enrichment; targeted N-glycopeptide quantification; lactation

资金

  1. Netherlands Organization for Scientific Research (NWO) [184.032.201]
  2. NWO TOP-Punt Grant [718.015.003]
  3. EU Horizon 2020 program INFRAIA project Epic-XS [823839]
  4. Chinese Scholarship Council (CSC)
  5. Danone Nutricia Research

向作者/读者索取更多资源

Protein N-glycosylation on human milk proteins assists in protecting an infant's health and functions among others as competitive inhibitors of pathogen binding and immunomodulators. Due to the individual uniqueness of each mother's milk and the overall complexity and temporal changes of protein N-glycosylation, analysis of the human milk N-glycoproteome requires longitudinal personalized approaches, providing protein- and N-site-specific quantitative information. Here, we describe an automated platform using hydrophilic-interaction chromatography (HILIC)-based cartridges enabling the proteome-wide monitoring of intact Nglycopeptides using just a digest of 150 mu g of breast milk protein. We were able to map around 1700 glycopeptides from 110 glycoproteins covering 191 glycosites, of which 43 sites have not been previously reported with experimental evidence. We next quantified 287 of these glycopeptides originating from 50 glycoproteins using a targeted proteomics approach. Although each glycoprotein, N-glycosylation site, and attached glycan revealed distinct dynamic changes, we did observe a few general trends. For instance, fucosylation, especially terminal fucosylation, increased across the lactation period. Building on the improved glycoproteomics approach outlined above, future studies are warranted to reveal the potential impact of the observed glycosylation microheterogeneity on the healthy development of infants.

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