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An enrichment method based on synergistic and reversible covalent interactions for large-scale analysis of glycoproteins

机译:一种基于协同和可逆共价键相互作用的富集方法,用于糖蛋白的大规模分析

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Protein glycosylation is ubiquitous in biological systems and essential for cell survival. However, the heterogeneity of glycans and the low abundance of many glycoproteins complicate their global analysis. Chemical methods based on reversible covalent interactions between boronic acid and glycans have great potential to enrich glycopeptides, but the binding affinity is typically not strong enough to capture low-abundance species. Here, we develop a strategy using dendrimer-conjugated benzoboroxole to enhance the glycopeptide enrichment. We test the performance of several boronic acid derivatives, showing that benzoboroxole markedly increases glycopeptide coverage from human cell lysates. The enrichment is further improved by conjugating benzoboroxole to a dendrimer, which enables synergistic benzoboroxole–glycan interactions. This robust and simple method is highly effective for sensitive glycoproteomics analysis, especially capturing low-abundance glycopeptides. Importantly, the enriched glycopeptides remain intact, making the current method compatible with mass-spectrometry-based approaches to identify glycosylation sites and glycan structures.
机译:蛋白质糖基化在生物系统中无处不在,对于细胞存活至关重要。然而,聚糖的异质性和许多糖蛋白的低丰度使它们的整体分析复杂化。基于硼酸和聚糖之间可逆的共价相互作用的化学方法具有丰富糖肽的巨大潜力,但结合亲和力通常不足以捕获低丰度物种。在这里,我们开发了一种使用树枝状大分子共轭苯并硼唑增强糖肽富集的策略。我们测试了几种硼酸衍生物的性能,表明苯并硼唑显着增加了人细胞裂解液中糖肽的覆盖率。通过将苯并硼烷与树状大分子缀合,可进一步提高富集度,从而实现苯并硼烷与聚糖的协同作用。这种鲁棒而简单的方法对于灵敏的糖蛋白组学分析,尤其是捕获低丰度糖肽,非常有效。重要的是,富集的糖肽保持完整,使当前方法与基于质谱的方法相兼容,以鉴定糖基化位点和聚糖结构。

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