ABSTRACT
Clone CL B5 of Trypanosoma cruzi is a beta-galactosidase expressing organism that was genetically transfected to be used for in vitro pharmacological screening. Biological parameters were determined, evaluating growth kinetics of epimastigotes, metacyclogenesis, infectivity to mammalian cell lines, parasitemia kinetics in mice and sensibility to nifurtimox and benznidazole. Differences in relation to other strains and CL parental strain were found, the most important being the incapability to produce death to mice in spite of the high inoculum used. However, it possesses the required features to be used for in vitro drug screening. Data obtained demonstrate that heterogeneity of T. cruzi appears even among clones of the same strain, and that these differences found do not prevent the use of clone CL B5 for the purpose that was engineered
Subject(s)
Animals , Mice , beta-Galactosidase , Trypanosoma cruzi , beta-Galactosidase , Cloning, Organism , Nifurtimox , Nitroimidazoles , Parasitemia , Parasitic Sensitivity Tests , Trypanocidal Agents , Trypanosoma cruziABSTRACT
Cytotoxicity assays of 24 new 3,5-disubstituted-tetrahydro-2H-1,3,5-thiadiazin-2-thione derivatives were performed. The 17 compounds with higher anti-epimastigote activity and lower cytotoxicity were, thereafter, screened against amastigote of Trypanosoma cruzi. Out of these 17 derivatives S-2d was selected to be assayed in vivo, because of its remarkable trypanocidal properties. To determine toxicity against J774 macrophages, a method based on quantification of cell damage, after 24 h, was used. Cell respiration, an indicator of cell viability, was assessed by the reduction of MTT [3-(4,5-dimethylthiazol-2-yl)-2,5-diphenyltetrazolium bromide] to formazan. Anti-amastigote activity was estimated after 48 h by microscopic counts of May Grünwald-Giemsa-stained monolayers. Nifurtimox and benznidazole were used as reference drugs. For the in vivo experiences, mice were infected with 10(4) blood trypomastigotes and then treated during 15 days with S-2d or nifurtimox by oral route. All of the compounds were highly toxic at 100 µg/ml for macrophages and a few of them maintained this cytotoxicity even at 10 µg/ml. Of the derivatives assayed against amastigotes 3k and S-2d showed an interesting activity, that was held even at 1µg/ml. It is demonstrated that the high anti-epimastigote activity previously reported is mainly due to the non-specific toxicity of these compounds. In vivo assays assessed a reduction of parasitemia after administration of S-2d to infected mice
Subject(s)
Animals , Mice , Antiprotozoal Agents , Macrophages , Thiadiazines , Trypanosoma cruzi , Antiprotozoal Agents , ThiadiazinesABSTRACT
Foram ensaiados, frente a uma cepa boliviana de Trypanosoma cruzi, dois novos derivados trifenilmetânicos obtidos por síntese: T-7A, bis (4-dimetilamino-fenil) 2-benzotienil carbinol e T-7B, tetrafluorborato de bis (4-dimetilamino - fenil) 2-benzotienil carbonio. As experiências foram realizadas em camundongos NMRI através da administraçäo dos produtos por via intraperitoneal. Foram realizados, também, testes de atividade tripanomicida, in vitro, com sangue contaminado e conservado sob refrigeraçäo