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Scalable Asymmetric Synthesis of the All Triamino Cyclohexane Core of BMS-813160.

作者信息

La Cruz Thomas E, González-Bobes Francisco, Eastgate Martin D, Sfouggatakis Chris, Zheng Bin, Kopp Nathaniel, Xiao Yi, Fan Yu, Galindo Kay A, Pathirana Charles, Galella Michael A, Deerberg Joerg

机构信息

Chemical Process Development, Bristol Myers Squibb, One Squibb Drive, New Brunswick, New Jersey 08903-0191, United States.

Analytical Strategy & Operations, Bristol Myers Squibb, One Squibb Drive, New Brunswick, New Jersey 08903-0191, United States.

出版信息

J Org Chem. 2022 Feb 18;87(4):1996-2011. doi: 10.1021/acs.joc.1c01162. Epub 2021 Aug 6.

DOI:10.1021/acs.joc.1c01162
PMID:34355895
Abstract

BMS-813160 is a pharmaceutical entity currently in development at Bristol Myers Squibb. Its defining structural feature is a unique chiral all triamino cyclohexane core. Medicinal and process chemistry groups at BMS have previously published synthesis strategies for chemotypes similar to the target molecule, but a streamlined approach amenable for longer-term supply was necessary. A new synthetic route was conceptualized, experimentally investigated, and determined to meet the criteria for efficiency that addressed key limitations of previous approaches. Adopting/optimizing the Trost asymmetric allylic amination desymmetrization methodology was a key tool used to produce a synthesis intermediate with high optical purity. In addition, developing a tandem Mannich-aza-Michael reaction to obviate the need for a Curtis/acylation sequence and a novel reductive amination/thermal lactamization to circumvent Freidinger-type pyrrolidone preparation are some of the synthesis improvements that enabled access to the target molecule to fulfill long-term supply requirements.

摘要

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