Publication Type Journal Article
Title Pharmacophore insights into rpoB gene mutations in Mycobacterium tuberculosis rifampicin resistant isolates
Authors Ricardo Figueiredo Daniela F. Ramos C. M. M. Moiteiro Maria Augusta Medeiros Maria Joao Marcelo Curto Jose Cardoso de Menezes Rogelio Hernandez Pando Pedro E. A. Silva Maria do Ceu Costa
Groups HC
Journal EUROPEAN JOURNAL OF MEDICINAL CHEMISTRY
Year 2012
Month January
Volume 47
Number
Pages 186-193
Abstract This paper reports the susceptibility profile to rifabutin (RFB) 1 and six recently synthesized RFB analogs 3-8, of either rifampicin (RFP) susceptible Mycobacterium tuberculosis and resistant clinical isolates from two sources: Mexico and Brazil. Taking into account that about 95\% of M. tuberculosis strains resistant to RFP present mutations in the rpoB gene, with some of these mutations being determinant also to RFB resistance, the RFB analogs were screened for activity against a set of known RFP susceptible and resistant strains. N -Acetyl-RFB 5 and N -(undec-10 -enoyl)-RFB 8 showed the best results, in particular with mutations in the codon 516, 522 and 531 of the rpoB gene, and were therefore selected for in vivo assessment of their efficacy. Studies conducted with tuberculous Balb/C mice previously infected with Ser531Leu mutated clinical isolate, evidenced both 5 and 8 as promoters of a significant decrease on tubercle bacilli burden in lungs associated with lower tissue damage, thus confirming them as good leads for drug discovery. The SAR of the acylated compounds 5 and 8 envisaging the identification of pharmacophore features, highlights the importance of profiling more clearly the chemistry within the molecular aspects for elucidation of the mode of action of RFB and analogs, in relation to mutations in Multidrug-Resistant (MDR) strains. (C) 2011 Elsevier Masson SAS. All rights reserved.
DOI http://dx.doi.org/10.1016/j.ejmech.2011.10.041
ISBN
Publisher
Book Title
ISSN 0223-5234
EISSN
Conference Name
Bibtex ID ISI:000301169800020
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