Discovery of Heterocyclic Replacements for the Coumarin Core of Anti-Tubercular FadD32 Inhibitors.

Chao Fang,Katie K. Lee,Raymond Nietupski,Robert H. Bates,Raquel Fernandez-Menendez,Eva Maria Lopez-Roman,Laura Guijarro-Lopez,Yunxing Yin, Zuozhong Peng,James E. Gomez,Stewart Fisher,David Barros-Aguirre,Brian K. Hubbard,Michael H. Serrano-Wu,Deborah T. Hung

BIOORGANIC & MEDICINAL CHEMISTRY LETTERS（2018）

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摘要

Previous work established a coumarin scaffold as a starting point for inhibition of Mycobacterium tuberculosis (Mtb) FadD32 enzymatic activity. After further profiling of the coumarin inhibitor 4 revealed chemical instability, we discovered that a quinoline ring circumvented this instability and had the advantage of offering additional substitution vectors to further optimize. Ensuing SAR studies gave rise to quinoline-2-carboxamides with potent anti-tubercular activity. Further optimization of ADME/PK properties culminated in 21b that exhibited compelling in vivo efficacy in a mouse model of Mtb infection.

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关键词

Mycobacterium tuberculosis,FadD32 inhibitor,Structure-activity relationship,Quinoline-2-carboxamide,In vivo efficacy

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