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神经细胞糖萼的代谢通量分析揭示了单糖的差异利用。

Metabolic flux analysis of the neural cell glycocalyx reveals differential utilization of monosaccharides.

机构信息

Department of Chemistry, University of California, Davis, Davis, CA 95616, USA.

Department of Anatomy, Physiology & Cell Biology, University of California, Davis, Davis, CA 95616, USA.

出版信息

Glycobiology. 2020 Oct 21;30(11):859-871. doi: 10.1093/glycob/cwaa038.

Abstract

Saccharides in our diet are major sources of carbon for the formation of biomass such as proteins, lipids, nucleic acids and glycans. Among the dietary monosaccharides, glucose occupies a central role in metabolism, but human blood contains regulated levels of other monosaccharides as well. Their influence on metabolism and how they are utilized have not been explored thoroughly. Applying metabolic flux analysis on glycan synthesis can reveal the pathways that supply glycosylation precursors and provide a snapshot of the metabolic state of the cell. In this study, we traced the incorporation of six 13C uniformly labeled monosaccharides in the N-glycans, O-glycans and glycosphingolipids of both pluripotent and neural NTERA-2 cells. We gathered detailed isotopologue data for hundreds of glycoconjugates using mass spectrometry methods. The contributions of de novo synthesis and direct incorporation pathways for glucose, mannose, fructose, galactose, N-acetylglucosamine and fucose were determined based on their isotope incorporation. Co-feeding studies revealed that fructose incorporation is drastically decreased by the presence of glucose, while mannose and galactose were much less affected. Furthermore, increased sialylation slowed down the turnover of glycans, but fucosylation attenuated this effect. Our results demonstrated that exogenous monosaccharide utilization can vary markedly depending on the cell differentiation state and monosaccharide availability, and that the incorporation of carbons can also differ among different glycan structures. We contend that the analysis of metabolic isotope labeling of glycans can yield new insights about cell metabolism.

摘要

我们饮食中的糖类是形成蛋白质、脂质、核酸和聚糖等生物量的主要碳源。在膳食单糖中,葡萄糖在代谢中占据核心地位,但人体血液中也含有调节水平的其他单糖。它们对代谢的影响以及它们的利用方式尚未得到充分探索。应用糖基化合成代谢通量分析可以揭示提供糖基化前体的途径,并提供细胞代谢状态的快照。在这项研究中,我们追踪了六种 13C 均匀标记的单糖在多能性和神经 NTERA-2 细胞的 N-聚糖、O-聚糖和糖脂中的掺入情况。我们使用质谱方法收集了数百种糖缀合物的详细同位素类似物数据。基于同位素掺入,确定了葡萄糖、甘露糖、果糖、半乳糖、N-乙酰葡萄糖胺和岩藻糖的从头合成和直接掺入途径的贡献。共喂养研究表明,葡萄糖的存在大大降低了果糖的掺入,而甘露糖和半乳糖的影响则较小。此外,唾液酸化的增加会减缓聚糖的周转率,但岩藻糖基化会减弱这种效应。我们的结果表明,外源性单糖的利用可能因细胞分化状态和单糖可用性而异,并且不同聚糖结构之间的碳掺入也可能不同。我们认为,糖基代谢同位素标记分析可以为细胞代谢提供新的见解。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/1af8/7581652/6b64b25d6296/cwaa038f1.jpg

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