Protein glycosylation regulates essential cellular processes such as signaling, adhesion and cell-cell interactions; however, dysregulated glycosylation is associated with diseases such as cancer. Here we introduce deep quantitative glycoprofiling (DQGlyco), a robust method that integrates high-throughput sample preparation, highly sensitive detection and precise multiplexed quantification to investigate protein glycosylation dynamics at an unprecedented depth. Using DQGlyco, we profiled the mouse brain glycoproteome, identifying 177,198 unique N-glycopeptides-25 times more than previous studies. We quantified glycopeptide changes in human cells treated with a fucosylation inhibitor and characterized surface-exposed glycoforms. Furthermore, we analyzed tissue-specific glycosylation patterns in mice and demonstrated that a defined gut microbiota substantially remodels the mouse brain glycoproteome, shedding light on the link between the gut microbiome and brain protein functions. Additionally, we developed a novel strategy to evaluate glycoform solubility, offering new insights into their biophysical properties. Overall, the in-depth profiling offered by DQGlyco uncovered extensive complexity in glycosylation regulation.
Uncovering protein glycosylation dynamics and heterogeneity using deep quantitative glycoprofiling (DQGlyco).
利用深度定量糖基化分析(DQGlyco)揭示蛋白质糖基化动态和异质性
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作者:Potel Clément M, Burtscher Mira Lea, Garrido-Rodriguez Martin, Brauer-Nikonow Amber, Becher Isabelle, Le Sueur Cecile, Typas Athanasios, Zimmermann Michael, Savitski Mikhail M
| 期刊: | Nature Structural & Molecular Biology | 影响因子: | 10.100 |
| 时间: | 2025 | 起止号: | 2025 Jun;32(6):1111-1126 |
| doi: | 10.1038/s41594-025-01485-w | 研究方向: | 免疫/内分泌 |
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