ABSTRACT
Nitroimidazoles exhibit high microbicidal activity, but mutagenic, genotoxic and cytotoxic properties have been attributed to the presence of the nitro group. However, we synthesised nitroimidazoles with activity against the trypomastigotes of Trypanosoma cruzi, but that were not genotoxic. Herein, nitroimidazoles (11-19) bearing different substituent groups were investigated for their potential induction of genotoxicity (comet assay) and mutagenicity (Salmonella/Microsome assay) and the correlations of these effects with their trypanocidal effect and with megazol were investigated. The compounds were designed to analyse the role played by the position of the nitro group in the imidazole nucleus (C-4 or C-5) and the presence of oxidisable groups at N-1 as an anion receptor group and the role of a methyl group at C-2. Nitroimidazoles bearing NO2 at C-4 and CH3 at C-2 were not genotoxic compared to those bearing NO 2 at C-5. However, when there was a CH3 at C-2, the position of the NO2 group had no influence on the genotoxic activity. Fluorinated compounds exhibited higher genotoxicity regardless of the presence of CH3 at C-2 or NO2 at C-4 or C-5. However, in compounds 11 (2-CH3; 4-NO2; N-CH2OHCH2Cl) and 12 (2-CH3; 4-NO2; N-CH2OHCH2F), the fluorine atom had no influence on genotoxicity. This study contributes to the future search for new and safer prototypes and provide.
Subject(s)
Animals , Mice , DNA Damage/drug effects , Nitroimidazoles/chemistry , Nitroimidazoles/toxicity , Salmonella/drug effects , Trypanosoma cruzi/drug effects , Comet Assay , Dose-Response Relationship, Drug , Mutagenicity Tests , Structure-Activity RelationshipABSTRACT
In this "Critical Review" we made a historical introduction of drugs assayed against Chagas disease beginning in 1912 with the works of Mayer and Rocha Lima up to the experimental use of nitrofurazone. In the beginning of the 70s, nifurtimox and benznidazole were introduced for clinical treatment, but results showed a great variability and there is still a controversy about their use for chronic cases. After the introduction of these nitroheterocycles only a few compounds were assayed in chagasic patients. The great advances in vector control in the South Cone countries, and the demonstration of parasite in chronic patients indicated the urgency to discuss the etiologic treatment during this phase, reinforcing the need to find drugs with more efficacy and less toxicity. We also review potential targets in the parasite and present a survey about new classes of synthetic and natural compounds studied after 1992/1993, with which we intend to give to the reader a general view about experimental studies in the area of the chemotherapy of Chagas disease, complementing the previous papers of Brener (1979) and De Castro (1993)
Subject(s)
Humans , Chagas Disease , Trypanocidal AgentsABSTRACT
Phenothiazines were observed to have a direct effect on Trypanosoma cruzi and on its in vitro interaction with host cells. They caused lysis of trypomastigotes (50 uM/24 h) and,to a lesser extent, epimastigote proliferation. Treatment of infected peritoneal macrophages with 12.5 uM chlorpromazine or triflupromazine inhibited the infection; this effect was found to be partially reversible if the drugs were removed after 24 h of treatment. At 60 uM, the drugs caused damage to amastigotes interiorized in heart muscle cells. However, the narrow margin of toxity between anti-trypanossomal activity and damage to host cells mitigates against in vivo investigation at the present time. Possible hypothesis for the mechanism of action of phenothiazines are discussed
Subject(s)
Animals , Phenothiazines/administration & dosage , Host-Parasite Interactions , Trypanosoma cruzi/drug effectsABSTRACT
The biosynthetic pigment from Chromobacterium violaceum BB-78, 1,3-dihydro-2H-indol-2-one and its derivatives exhibit biological activities such as antimicrobial action, low hemolytic effects on red blood cells and in vitro trypanocide activity. A relatively high cytotoxicity on V-79 hamster fibroblast cells of the biosynthetic pigment was found, although with the methylol derivative the toxicity was almost eliminated. The methylol derivative exhibited similar toxicity as Nifurtimox, a known, commercial trypanocide compound
Subject(s)
Animals , Cricetinae , Anti-Bacterial Agents/toxicity , Chromobacterium/metabolism , Hemolysis , Indoles/toxicity , Pigments, Biological/toxicity , Anti-Bacterial Agents/isolation & purification , Bacteria/drug effects , Cell Line , Cell Survival/drug effects , Chromobacterium/growth & development , Fibroblasts/drug effects , Indoles/isolation & purification , Microbial Sensitivity Tests , Nifurtimox/toxicity , Pigments, Biological/isolation & purification , Trypanosoma cruzi/drug effects , Trypanosoma cruzi/growth & developmentABSTRACT
Megazol (CL 64,855) a very effective drug in experimental infections by Trypanosoma cruzi, and also in in vitro assays with vertebrate forms of the parasite, had its parasite, had its activity upon macromolecule biosynthesis tested using tissue culture-derived amastigote forms. Megazol presented a drastic inhibition of [3H]-uridine incorporation, suggesting a selective activity upon protein synthesis. Comparing the three drugs, megazol was more potent than nifurtimox and benznidazole in inhibiting protein an DNA synthesis. Megazol showed a 91% of inhibition of [3H]-leucine incorporation whereas nifurtimox and benznidazole, 0% and 2%, respectively. These latter two drugs inhibited the incorporation of all the precursors tested at similar levels, but the concentration of benznidazole was always three times higher, suggesting different mechanisms of action or, more probably, a greater efficiency of the 5-nitrofuran derivate in relation to the 2-nitroimidazole. So, wes conclude that the mode of action of megazol is different from the ones of nifurtimox and benznidazole and that its primary effect is associated with an impairment of protein synthesis
Subject(s)
Animals , In Vitro Techniques , Nitroimidazoles/pharmacology , Proteins/biosynthesis , Thiadiazoles/pharmacology , Trypanosoma cruzi/drug effects , Benzimidazoles/pharmacology , Drug Combinations , Leucine/metabolism , Nifurtimox/pharmacologyABSTRACT
As açöes de megazol, nifurtimox, benznidazol e allopurinol sobre o T. cruzi foram investigadas, através de microscopia ótica e eletrônica, pela análise do efeito direto sobre formas amastigotas e tripomastigotas e do efeito sobre a interaçäo de cultura de célula muscular cardíaca com tripomastigotas sangüíneos. A proliferaçäo de amastigotas em meio Warren foi inibida de modo dose-dependente por megazol, nifurtimox e benznidazol. O tratamento de amastigotas (25-50 micronM/24h) e de tripomastigotas (25 micronM/24h) levou a várias alteraçöes ultraestruturais nos parasitas. Estas três drogas tiveram também um efeito potente no tratamento de culturas de células cardíacas infectadas, quando adicionadas desde o início da interaçäo ou após um ou três dias de infecçäo. Os parasitas interiorizados mostraram um padräo de alteraçöes ultraestruturais semelhante ao observado no tratamento direto de formas amastigotas. A cultura primária de célula muscular cardíaca mostrou ser um modelo adequado para o estudo de drogas sobre formas intracelulares de T. cruzi e o ensaio de proliferaçäo de amastigotas em meio axênico, indicado para uma triagem inicial de drogas. Estes parâmetros nos parecem muito confiáveis para uma investigaçäo sistemática do mecanismo de açäo de drogas