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Toward a Molecular Lego Approach for the Diversity-Oriented Synthesis of Cyclodextrin Analogues Designed as Scaffolds for Multivalent Systems

机译:面向分子乐高方法的面向多样性的合成设计为多价体系支架的环糊精类似物

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摘要

A modular strategy has been developed to access a diversity of cyclic and acyclic oligosaccharide analogues designed as prefunctionalized scaffolds for the synthesis of multivalent ligands. This convergent approach is based on bifunctional sugar building blocks with two temporarily masked functionalities that can be orthogonally activated to perform Cu(I)-catalyzed azide-alkyne cycloaddition reactions (CuAAC). The reducing end is activated as a glycosyl azide and masked as a 1,6-anhydro sugar, while the nonreducing end is activated as a free alkyne and masked as a triethylsilyl-alkyne. Following a cyclooligomerization approach, the first examples of close analogues of cyclodextrins composed of D-glucose residues and triazole units bound together through alpha-(1,4) linkages were obtained. The cycloglucopyranoside analogue containing four sugar units was used as a template to prepare multivalent systems displaying a protected D-mannose derivative or an iminosugar by way of CuAAC. On the other hand, the modular approach led to acyclic alkyne-functionalized scaffolds of a controlled size that were used to synthesize multivalent iminosugars.
机译:已经开发了模块化策略以访问设计为预功能化支架的,用于合成多价配体的多种环状和无环寡糖类似物。这种收敛方法基于具有两个暂时掩盖的功能的双功能糖结构单元,该功能可以被正交激活以执行Cu(I)催化的叠氮化物-炔烃环加成反应(CuAAC)。还原端被活化为糖基叠氮化物并被掩蔽为1,6-脱水糖,而非还原端被活化为游离炔基并被掩蔽为三乙基甲硅烷基炔。按照环寡聚化方法,获得了由D-葡萄糖残基和三唑单元通过α-(1,4)键结合在一起的环糊精的紧密类似物的第一个例子。使用含有四个糖单元的环吡喃葡萄糖苷类似物作为模板,以制备通过CuAAC展示受保护的D-甘露糖衍生物或亚氨基糖的多价系统。另一方面,模块化方法导致了大小可控的无环炔烃官能化支架,用于合成多价亚氨基糖。

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