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一种中大型糖类似物的迁徙性以太形成途径。

A Migratory Ether Formation Route to Medium-Sized Sugar Mimetics.

机构信息

Key Laboratory of Chemical Genomics, Peking University Shenzhen Graduate School, Shenzhen, 518055, China.

School of Chemical Engineering, Shandong University of Technology, Zibo, 255049, P. R. China.

出版信息

Angew Chem Int Ed Engl. 2016 Nov 7;55(46):14340-14344. doi: 10.1002/anie.201608974. Epub 2016 Oct 13.

Abstract

Polyol-substituted cyclic ethers are fundamental building blocks of biomolecules. The position and stereochemistry of multiple hydroxy substituents of cyclic ethers play a central role in their biological function. Current methods for the synthesis of such structures are limited to "naked" ring products with no or few substituents. Here we describe a general route to medium-sized polyol cyclic ethers using a migratory ether formation strategy. In contrast to the common pathway of direct opening of epoxides, Me Al was found to promote an unprecedented ether addition reaction, opening a neighboring epoxide. The resulting oxonium intermediate triggers a 1,3-methyl shift to yield 2-deoxyribital products. When the hemiacetal auxiliary is a monosaccharide, the sugar ring is expanded by four atoms to give the corresponding 9- to 11-membered analogues. This method provides an entry into the untapped chemical space of medium-sized sugar mimetics.

摘要

多元醇取代的环醚是生物分子的基本结构单元。环醚中多个羟基取代基的位置和立体化学在其生物功能中起着核心作用。目前合成此类结构的方法仅限于“裸露”的环产物,几乎没有或只有少数取代基。在这里,我们描述了一种使用迁移醚形成策略合成中等大小多元醇环醚的通用方法。与直接开环环氧化物的常见途径不同,我们发现 Me Al 可以促进前所未有的醚加成反应,打开相邻的环氧化物。所得的氧鎓中间体引发 1,3-甲基迁移,生成 2-脱氧核糖产物。当半缩醛辅助物是单糖时,糖环通过四个原子扩展,得到相应的 9-至 11 元类似物。该方法为中等大小糖类似物的未开发化学空间提供了切入点。

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