New insight into structure-activity of furan-based salicylate synthase (MbtI) inhibitors as potential antitubercular agents
Laurent R. Chiarelli, Matteo Mori, Giangiacomo Beretta, Arianna Gelain, Elena Pini, Josè Camilla Sammartino, Giovanni Stelitano, Daniela Barlocco, et al. (17 authors)
Journal of Enzyme Inhibition and Medicinal Chemistry · 2019-01
Abstract
Starting from the analysis of the hypothetical binding mode of our previous furan-based hit (I), we successfully achieved our objective to replace the nitro moiety, leading to the disclosure of a new lead exhibiting a strong activity against MbtI. Our best candidate 1 h displayed a Ki of 8.8 µM and its antimycobacterial activity (MIC99 = 250 µM) is conceivably related to mycobactin biosynthesis inhibition. These results support the hypothesis that 5-phenylfuran-2-carboxylic derivatives are a promising class of MbtI inhibitors.
MeSH terms
- Moiety
- Furan
- Chemistry
- Stereochemistry
- Biosynthesis
- Antimycobacterial
- Pharmacology
- ATP synthase
- Structure–activity relationship
- Biochemistry
- Enzyme
- Combinatorial chemistry