Activity Of (-)-Camphene Derivatives Against Mycobacterium tuberculosis In Acidic pH.

Activity Of (-)-Camphene Derivatives Against Mycobacterium tuberculosis In Acidic pH.

de Carvalho, Hayalla Corrêa;Ieque, Andressa Lorena;Valverde, Tamires Leite;Baldin, Vanessa Pietrowski;Meneguello, Jean Eduardo;Campanerut-Sá, Paula Aline Zanetti;Vandresen, Fábio;Ghiraldi Lopes, Luciana Dias;Passos Souza, Mariana Regina;Santos, Nathally Claudiane de Souza;Dias Siqueira, Vera Lucia;Caleffi-Ferracioli, Katiany Rizzieri;Lima Scodro, Regiane Bertin;Cardoso, Rosilene Fressatti;
medicinal chemistry (shariqah (united arab emirates)) 2019
253
de-carvalho2019activitymedicinal

Abstract

For more than 60 years, the lack of new anti-tuberculosis drugs and the increase of resistant Mycobacterium tuberculosis lineages exhibit a therapeutic challenge, demanding new options for the treatment of resistant tuberculosis.Herein, we determined the (i) activities of (-)-camphene and derivatives and (ii) combinatory effect with pyrazinamide (PZA) against Mycobacterium tuberculosis in acidic pH and (iii) cytotoxicity in VERO cells.The activity of (-)-camphene and 15 derivatives were determined in M. tuberculosis H37Rv in culture medium at pH 6.0 by Resazurin Microtiter Assay Plate (REMA). The combinatory study of three (-)-camphene derivatives with PZA was carried out in seven multidrug-resistant (MDR) clinical isolates by REMA and Checkerboard, respectively. The assay of 3-(4,5-dimethylthiazol-2-yl)-2,5-diphenyltetrazolium (MTT) bromide in VERO cells was used to determine the derivatives cytotoxicity.Four (-)-Camphene derivatives, (4), (5a) (5d) and (5h), showed reduction in MIC value at pH 6.0 compared to MIC detected at pH 6.8 in M. tuberculosis H37Rv and multidrug resistant clinical isolates. Three (-)-camphene derivatives, (4), (5d) and (5h), showed synergistic effect (FICI ≤ 0.5) combined with PZA and were more selective for M. tuberculosis than VERO cell (selective index from 7.7 to 84.2).Three (-)-camphene derivatives have shown to be promising anti-TB molecule scaffold due to the low MIC values in acidic pH against MDR M. tuberculosis clinical isolates, synergism with PZA and low cytotoxicity.

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75485
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10.2174/1573406415666191106124016
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