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Exploration of the use of an acylsulfonamide safety-catch linker for the polymer-supported synthesis of hyaluronic acid oligosaccharides

机译:探索酰基磺酰胺安全捕捉连接子在聚合物支持的透明质酸低聚糖合成中的应用

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摘要

The synthesis of hyaluronic acid oligosaccharides on polyethylene glycol (PEG) using an acylsulfonamide linker has been explored. Hyaluronic acid is a challenging synthetic target that usually involves the condensation of highly disarmed glucuronic acid building blocks. Amine-ended PEG monomethyl ether was efficiently functionalized with a hydroxyl-terminated acylsulfonamide linker. Suitably protected D-glucosamine (GlcN) and n-glucuronic acid (GlcA) monosaccharide building blocks were coupled to the polymer acceptor using the trichloroacetimidate glycosylation method. The sulfonamide safety-catch linker enables simultaneous cleavage of the monosaccharide from the polymer and orthogonal functionalization for further (bio)-conjugation of the sugar sample. Subsequent glycosylation of PEG-bound glycosyl acceptor to generate hyaluronic acid oligosaccharide chain failed. Model glycosylation experiments in solution and on soluble support using the same unreactive acceptors and donors allows for the synthesis of an orthogonally protected hyaluronic acid disaccharide and suggest that the encountered difficulties could be attributed to the presence of the N-acylsulfonamide.
机译:已经研究了使用酰基磺酰胺连接基在聚乙二醇(PEG)上合成透明质酸寡糖。透明质酸是具有挑战性的合成目标,通常涉及高度分解的葡萄糖醛酸构建基团的缩合。胺端的PEG单甲醚已被羟基封端的酰基磺酰胺连接基有效地官能化。使用三氯乙亚氨酸酯糖基化方法,将适当保护的D-葡萄糖胺(GlcN)和正葡萄糖醛酸(GlcA)单糖结构单元与聚合物受体偶联。磺酰胺安全捕捉接头可同时从聚合物上裂解单糖并进行正交官能化,以使糖样品进一步(生物)结合。随后的PEG结合的糖基受体的糖基化生成透明质酸寡糖链失败。使用相同的非反应性受体和供体,在溶液中和在可溶性支持物上进行模型糖基化实验,可以合成正交保护的透明质酸二糖,并表明遇到的困难可能归因于N-酰基磺酰胺的存在。

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