| Literature DB >> 26142487 |
Aurélien Chollet1, Giorgia Mori2, Christophe Menendez3, Frédéric Rodriguez3, Isabelle Fabing3, Maria Rosalia Pasca2, Jan Madacki4, Jana Korduláková4, Patricia Constant5, Annaïk Quémard5, Vania Bernardes-Génisson6, Christian Lherbet7, Michel Baltas3.
Abstract
A series of fluorene-based derivatives was synthesized and evaluated for inhibiting both InhA and Mycobacterium tuberculosis growth. These compounds were inspired by the previously reported Genz-10850 molecule, a good InhA inhibitor, but with a poor activity against M. tuberculosis growth. Structure-activity relationships were performed by introducing the following chemical modifications: 1) the piperazine ring; 2) the amide group; 3) the aryl moiety; and 4) the fluorene moiety. Among these new derivatives, one of them was more effective against both the InhA activity and mycobacterial growth, compared to the hit compound. Docking studies were also performed to rationalize activities of these derivatives. Furthermore, we showed for the first time that efflux pump inhibitors potentiated the efficacy of Genz-10850 (GEQ) derivatives against M. tuberculosis growth, demonstrating that these compounds could be substrates of some efflux pumps.Entities:
Keywords: Efflux pumps; InhA; Inhibitors; Medicinal chemistry; Mycobacterium tuberculosis
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Year: 2015 PMID: 26142487 DOI: 10.1016/j.ejmech.2015.06.035
Source DB: PubMed Journal: Eur J Med Chem ISSN: 0223-5234 Impact factor: 6.514