Discovery of an Imine Reductase for Reductive Amination of Carbonyl Compounds with Sterically Challenging Amines

化学 位阻效应 亚胺 还原胺化 胺化 胺气处理 亲核细胞 组合化学 有机化学 烷基 催化作用
作者
Fei-Fei Chen,Xiao‐Ting He,Xin-Xin Zhu,Zhi Zhang,Xinyuan Shen,Qi Chen,Jian‐He Xu,Nicholas J. Turner,Gao‐Wei Zheng
出处
期刊:Journal of the American Chemical Society [American Chemical Society]
卷期号:145 (7): 4015-4025 被引量:21
标识
DOI:10.1021/jacs.2c11354
摘要

The synthesis of structurally diverse amines is of fundamental significance in the pharmaceutical industry due to the ubiquitous presence of amine motifs in biologically active molecules. Biocatalytic reductive amination for amine production has attracted great interest owing to its synthetic advantages. Herein, we report the direct synthesis of a wide range of sterically demanding secondary amines, including several important active pharmaceutical ingredients and pharmaceutical intermediates, via reductive amination of carbonyl substrates and bulky amine nucleophiles employing imine reductases. Key to success for this route is the identification of an imine reductase from Penicillium camemberti with unusual substrate specificity and its further engineering, which empowered the accommodation of a broad range of sterically demanding amine nucleophiles encompassing linear alkyl and (hetero)aromatic (oxy)alkyl substituents and the formation of final amine products with up to >99% conversion. The practical utility of the biocatalytic route has been demonstrated by its application in the preparative synthesis of the anti-hyperparathyroidism drug cinacalcet.
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