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可编程一锅法糖基化

Programmable one-pot glycosylation.

作者信息

Wu Chung-Yi, Wong Chi-Huey

机构信息

Genomics Research Center, Academia Sinica, Nankang, Taipei 115, Taiwan.

出版信息

Top Curr Chem. 2011;301:223-52. doi: 10.1007/128_2010_109.

Abstract

In oligosaccharide synthesis, protecting groups, possible participating groups, promoters/catalysts, reaction conditions, and donor leaving groups and acceptors must all be carefully designed in order to generate the correct regio- and stereochemistry for the new glycosidic bond. Programmable one-pot synthesis has been developed to address the above problems. This strategy is based on the sequential use of thioglycoside building blocks to form glycosidic bonds based on the reactivity difference of the building blocks. The activation of the anomeric leaving group can be attenuated through modification of the protecting group strategy and neighboring group participation. This reactivity-based strategy has been applied to one-pot glycosylation reactions where a series of building blocks with identical leaving groups react sequentially in one vessel without laborious intermediate purification steps. It provides rapid access to oligosaccharides with a wide-range of molecular diversity. In this chapter we outline the recent development of this strategy that can be applied to synthesize a wide variety of oligosaccharides and glycoconjugates that are associated with infectious diseases or carbohydrate-based cancer antigens.

摘要

在低聚糖合成中,保护基、可能的参与基团、促进剂/催化剂、反应条件以及供体离去基团和受体都必须经过精心设计,以便为新的糖苷键生成正确的区域化学和立体化学。为了解决上述问题,已开发出可编程的一锅法合成。该策略基于硫代糖苷构建块的顺序使用,根据构建块的反应性差异形成糖苷键。异头离去基团的活化可通过保护基策略的修饰和邻基参与来减弱。这种基于反应性的策略已应用于一锅法糖基化反应,其中一系列具有相同离去基团的构建块在一个容器中顺序反应,无需繁琐的中间纯化步骤。它提供了快速获取具有广泛分子多样性的低聚糖的途径。在本章中,我们概述了该策略的最新进展,该策略可用于合成与传染病或基于碳水化合物的癌症抗原相关的多种低聚糖和糖缀合物。

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