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A synthetic approach to ‘click’ neoglycoprotein analogues of EPO employing one-pot native chemical ligation and CuAAC chemistry

机译:一锅天然化学连接和CuAAC化学合成点击 EPO新糖蛋白类似物的合成方法

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摘要

The clinical significance of batch-wise variability on the pharmacokinetics and potency of commercial erythropoietin (EPO), prepared recombinantly as a heterogeneous mixture of glycoforms, necessitates the development of synthetic strategies to afford homogenous EPO formulations. Herein we present a previously unexplored and divergent route towards ‘click’ neoglycoprotein analogues of EPO, employing one-pot native chemical ligation (NCL) of alkynylated peptides and copper-catalysed azide–alkyne cycloaddition (CuAAC) with azido monosaccharides. By design, our synthetic platform permits glycosylation at virtually any stage, providing flexibility for the synthesis of various glycoforms for biological analysis. Insights obtained from attempted folding of our ‘click’ neoglycoprotein EPO analogue, bearing four different neutral sugar moieties, highlight the important role played by the charged oligosaccharides present in native EPO glycoproteins.
机译:以糖异质混合物的形式重组制备的商业促红细胞生成素(EPO)的药代动力学和效能的分批变异性的临床意义,有必要开发合成策略以提供均质的EPO制剂。本文中,我们提出了一种利用EPO的“点击”新糖蛋白类似物的先前未探索和分歧的途径,该方法采用了一锅化的烷基化肽的天然化学连接(NCL)和铜催化的叠氮基-炔烃环加成(CuAAC)与叠氮基单糖。通过设计,我们的合成平台几乎可以在任何阶段进行糖基化,从而为生物学分析中各种糖型的合成提供了灵活性。尝试折叠带有四个不同中性糖部分的“ click”新糖蛋白EPO类似物进行折叠获得的见解突显了天然EPO糖蛋白中带电寡糖发挥的重要作用。

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