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Applying Acylated Fucose Analogues to Metabolic Glycoengineering

机译:酰化岩藻糖类似物在代谢糖工程中的应用

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摘要

Manipulations of cell surface glycosylation or glycan decoration of selected proteins hold immense potential for exploring structure-activity relations or increasing glycoprotein quality. Metabolic glycoengineering describes the strategy where exogenously supplied sugar analogues intercept biosynthetic pathways and are incorporated into glycoconjugates. Low membrane permeability, which so far limited the large-scale adaption of this technology, can be addressed by the introduction of acylated monosaccharides. In this work, we investigated tetra-O-acetylated, -propanoylated and -polyethylene glycol (PEG)ylated fucoses. Concentrations of up to 500 µM had no substantial effects on viability and recombinant glycoprotein production of human embryonic kidney (HEK)-293T cells. Analogues applied to an engineered Chinese hamster ovary (CHO) cell line with blocked fucose de novo synthesis revealed an increase in cell surface and recombinant antibody fucosylation as proved by lectin blotting, mass spectrometry and monosaccharide analysis. Significant fucose incorporation was achieved for tetra-O-acetylated and -propanoylated fucoses already at 20 µM. Sequential fucosylation of the recombinant glycoprotein, achieved by the application of increasing concentrations of PEGylated fucose up to 70 µM, correlated with a reduced antibody’s binding activity in a Fcγ receptor IIIa (FcγRIIIa) binding assay. Our results provide further insights to modulate fucosylation by exploiting the salvage pathway via metabolic glycoengineering.
机译:对选定蛋白质进行细胞表面糖基化或聚糖修饰的操作具有探索结构-活性关系或提高糖蛋白质量的巨大潜力。代谢糖工程学描述了一种策略,其中外源提供的糖类似物拦截生物合成途径,并掺入糖缀合物中。膜渗透性低,迄今为止限制了该技术的大规模应用,可以通过引入酰化单糖来解决。在这项工作中,我们研究了四-O-乙酰化,-丙酰化和-聚乙二醇(PEG)化的胶浆。浓度高达500 µM对人胚肾(HEK)-293T细胞的活力和重组糖蛋白生产没有实质性影响。应用于凝集的岩藻糖合成的工程化中国仓鼠卵巢(CHO)细胞系的类似物显示,通过凝集素印迹,质谱和单糖分析证明,细胞表面和重组抗体岩藻糖基化程度增加。对于已经达到20 µM的四-O-乙酰化和-丙酰化的岩藻糖,可实现明显的岩藻糖掺入。通过增加浓度高达70 µM的聚乙二醇化岩藻糖可实现重组糖蛋白的顺序岩藻糖基化,这与Fcγ受体IIIa(FcγRIIIa)结合试验中抗体的结合活性降低有关。我们的结果为通过代谢糖工程利用挽救途径调节岩藻糖基化提供了进一步的见解。

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