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铜催化的对映选择性立体发散合成氨基醇。

Copper-catalysed enantioselective stereodivergent synthesis of amino alcohols.

作者信息

Shi Shi-Liang, Wong Zackary L, Buchwald Stephen L

机构信息

Department of Chemistry, Massachusetts Institute of Technology, Cambridge, Massachusetts 02139, USA.

出版信息

Nature. 2016 Apr 21;532(7599):353-6. doi: 10.1038/nature17191. Epub 2016 Mar 28.

Abstract

The chirality, or 'handedness', of a biologically active molecule can alter its physiological properties. Thus it is routine procedure in the drug discovery and development process to prepare and fully characterize all possible stereoisomers of a drug candidate for biological evaluation. Despite many advances in asymmetric synthesis, developing general and practical strategies for obtaining all possible stereoisomers of an organic compound that has multiple contiguous stereocentres remains a challenge. Here, we report a stereodivergent copper-based approach for the expeditious construction of amino alcohols with high levels of chemo-, regio-, diastereo- and enantioselectivity. Specifically, we synthesized these amino-alcohol products using sequential, copper-hydride-catalysed hydrosilylation and hydroamination of readily available enals and enones. This strategy provides a route to all possible stereoisomers of the amino-alcohol products, which contain up to three contiguous stereocentres. We leveraged catalyst control and stereospecificity simultaneously to attain exceptional control of the product stereochemistry. Beyond the immediate utility of this protocol, our strategy could inspire the development of methods that provide complete sets of stereoisomers for other valuable synthetic targets.

摘要

生物活性分子的手性,即“旋光性”,会改变其生理特性。因此,在药物发现和开发过程中,制备并全面表征候选药物的所有可能立体异构体以进行生物学评估是常规操作。尽管不对称合成取得了许多进展,但开发通用且实用的策略以获得具有多个相邻立体中心的有机化合物的所有可能立体异构体仍然是一项挑战。在此,我们报告了一种基于铜的立体发散方法,用于快速构建具有高化学、区域、非对映和对映选择性的氨基醇。具体而言,我们通过依次进行氢化铜催化的硅氢化反应和对易得的烯醛和烯酮进行氢胺化反应来合成这些氨基醇产物。该策略为氨基醇产物的所有可能立体异构体提供了一条途径,这些产物含有多达三个相邻立体中心。我们同时利用催化剂控制和立体专一性来实现对产物立体化学的出色控制。除了该方案的直接实用性之外,我们的策略还可能激发为其他有价值的合成目标提供完整立体异构体集的方法的开发。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/0beb/4844805/17a768ddb137/nihms755500f1.jpg

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