化学
兴奋剂
酮
还原(数学)
酶
部分激动剂
树枝状大分子
组合化学
有机化学
受体
生物化学
几何学
数学
作者
Alan M. Hyde,Zhijian Liu,Birgit Kosjek,Lushi Tan,Artis Klapars,Eric R. Ashley,Yong‐Li Zhong,Oscar Alvizo,Nicholas J. Agard,Guiquan Liu,Xiuyan Gu,Nobuyoshi Yasuda,John Limanto,Mark A. Huffman,David M. Tschaen
出处
期刊:Organic Letters
[American Chemical Society]
日期:2016-11-01
卷期号:18 (22): 5888-5891
被引量:33
标识
DOI:10.1021/acs.orglett.6b02910
摘要
A scalable and efficient synthesis of the GPR40 agonist MK-8666 was developed from a simple pyridine building block. The key step to set the stereochemistry at two centers relied on an enzymatic dynamic kinetic reduction of an unactivated ketone. Directed evolution was leveraged to generate an optimized ketoreductase that provided the desired trans alcohol in >30:1 dr and >99% ee. Further, it was demonstrated that all four diastereomers of this hydroxy-ester could be prepared in high yield and selectivity. Subsequently, a challenging intramolecular displacement was carried out to form the cyclopropane ring system with perfect control of endo/exo selectivity. The endgame coupling strategy relied on a Pd-catalyzed C-O coupling to join the headpiece chloropyridine with the benzylic alcohol tailpiece.
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