Journal
ORGANIC PROCESS RESEARCH & DEVELOPMENT
Volume 24, Issue 7, Pages 1294-1303Publisher
AMER CHEMICAL SOC
DOI: 10.1021/acs.oprd.0c00180
Keywords
glucokinase activator; diastereoselective epoxidation; one-pot synthesis; isomerization of alkene
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We describe the process research and development of a practical synthesis of glucokinase activator 1 as a potential drug for treating type 2 diabetes mellitus. The key structure, a 3,4-cis-difluorinated cyclopentane moiety, was constructed via diastereoselective epoxidation, followed by one-pot difluorination with Et3N center dot 3HF and perfluorobutanesulfonyl fluoride (PBSF). Julia olefination of benzothiazol-2-yl sulfone with glyoxylate furnished an E/Z mixture of acrylate, followed by isomerization of the alkene to the desired E configuration during the formation of the acid chloride in the final step. This development achieved a highly practical process route to 1 (15% overall yield, 12 steps). This process route overcomes the drawbacks of the original medicinal chemistry synthetic route, which used hazardous and costly reagents (LiAlH4, OsO4, and Deoxo-Fluor) and had low efficiency (<4% overall yield, 20 steps).
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