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Anti-Trypanosoma cruzi Activity of Metabolism Modifier Compounds
Authors:Nieves Martinez-Peinado  Clara Martori  Nuria Cortes-Serra  Julian Sherman  Ana Rodriguez  Joaquim Gascon  Jordi Alberola  Maria-Jesus Pinazo  Alheli Rodriguez-Cortes  Julio Alonso-Padilla
Affiliation:1.Barcelona Institute for Global Health (ISGlobal), Hospital Clínic—University of Barcelona, 08036 Barcelona, Spain; (N.M.-P.); (N.C.-S.); (J.G.); (M.-J.P.);2.Department of Pharmacology, Toxicology, and Therapeutics, Veterinary Faculty, Autonomous University of Barcelona, 08193 Bellaterra, Spain; (C.M.); (J.A.);3.Department of Microbiology, New York University School of Medicine, New York, NY 10010, USA; (J.S.); (A.R.)
Abstract:Chagas disease is caused by the protozoan parasite Trypanosoma cruzi and affects over 6 million people worldwide. Development of new drugs to treat this disease remains a priority since those currently available have variable efficacy and frequent adverse effects, especially during the long regimens required for treating the chronic stage of the disease. T. cruzi modulates the host cell-metabolism to accommodate the cell cytosol into a favorable growth environment and acquire nutrients for its multiplication. In this study we evaluated the specific anti-T. cruzi activity of nine bio-energetic modulator compounds. Notably, we identified that 17-DMAG, which targets the ATP-binding site of heat shock protein 90 (Hsp90), has a very high (sub-micromolar range) selective inhibition of the parasite growth. This inhibitory effect was also highly potent (IC50 = 0.27 μmol L−1) against the amastigote intracellular replicative stage of the parasite. Moreover, molecular docking results suggest that 17-DMAG may bind T. cruzi Hsp90 homologue Hsp83 with good affinity. Evaluation in a mouse model of chronic T. cruzi infection did not show parasite growth inhibition, highlighting the difficulties encountered when going from in vitro assays onto preclinical drug developmental stages.
Keywords:Trypanosoma cruzi  Chagas disease  metabolism drugs  phenotypic assays  cytotoxicity assays  chronic in vivo model  dorsomorphin  17-DMAG
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