Estudo da coagulação do sangue com o medicamento 1(5-Nitro-2-Tiazolil-2-Imidazolidinona) - Ciba 32.644-Ba: niridazol no tratamento da esquistossomose mansoni

Os autores estudaram a coagulação do sangue em 30 pacientes tratados com 25mg/kg/dia/7 dias, com o composto 1 (5-Nitro-2-Tiazolil-2-Imidazolidinona) - Ciba 32.644 - Ba. Além do exame clínico e várias provas laboratoriais, efetuaram pesquisa do tempo de protrombina, retração do coágulo, dosagem de fibrinogênio, contagem de plaquetas, tempo de sangria e coagulação. As alterações observadas não nos parecem ter influência nas hemorragias que possam ocorrer durante o tratamento com o medicamento estudado, em pacientes com a forma hepato-intestinal da esquistossomose. Mesmo a queda discreta do tempo de protrombina, verificada nos 6 meses seguintes ao tratamento, em seis dos pacientes, não favoreceria a hemorragia, porque os valores encontrados não alcançaram o limiar da mesma. Quanto à retração do coágulo, como alteração isolada, parece-nos impossível a interpretação de que possa ser justificada por alguma alteração na fisiologia das plaquetas.

Ultrastructural alterations of intracellular stages and effects on blood forms of Trypanosoma cruzi induced in vivo by 2-amino-5-(1-methyil-5-nitro-2-imidazolyl)-1,3,4 - Thiadiazole

An electron microscopy study shows that the administration of a single dose (500 mg/kg, p.o.) of 2-amino-5-(1-methyl-5-nitro-2-imidazolyl)-1, 3, 4-thiadiazole induces in mice infected with Trypanosoma cruzi results in degenerative lesions of the intracellular stages. Ultrastructural alterations are detected as early as 6 hours after the drug administration and destruction of the parasites occurs within 18 - 36 hours. Trypomastigotes are cleared from the bloodstream 4 to 6 hours after treatment. The combined effect on both developmental stages is apparently responsible for the in vivo ejfects of this drug which is the most active drug ever tested in our laboratory in experimental Chagas' disease.

In Vitro and in Vivo Anti-Trypanosoma cruzi Activity of a Novel Nitro-derivative

Nitroarylidenemalononitriles and their cyanoacetamide derivatives with remarkable anti-epimastigote properties, were synthesized attempting to obtain new 3,5-diamino-4-(5'-nitroarylidene)-4H-thiadiazine 1,1-dioxide derivatives, which in previous reports had shown anti-Trypanosoma cruzi activity. Tests to evaluate the cytotoxicity of compounds were performed on J774 macrophages. 5-nitro-2-thienyl-malononitrile (5NO2TM), was the only product which maintained a high anti-epimastigote activity at concentrations in which it was no longer cytotoxic, thus it was assayed against intracellular amastigotes. Its anti-amastigote activity was similar to that of nifurtimox. Afterwards in vivo toxicity and anti-chagasic activity were determined. A reduction in parasitemia was observed.

Studies of genotoxicity and mutagenicity of nitroimidazoles: demystifying this critical relationship with the nitro group

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 NO2 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.

Comportamento térmico do 8-quinolinol e seus nitro-derivados

The compounds 5-nitro-8-quinolinol and 5,7-dinitro-8-quinolinol were obtained by nitration of the chelant 8-quinolinol. The compounds were characterized through EA, MNR, XRD, IR, TG, DTA and DSC. It was verified through thermal analysis that the compounds show consecutive processes of sublimation, fusion and vaporization. During the vaporization process, partial thermal decomposition was observed, with formation of carbonaceous residues. Considering a slower heating rate, the sublimation is the prevalent process to the nitro-derivatives while the vaporization is the main process to 8-quinolinol. The thermal stability follows the decreasing order from 5,7-dinitro-8-quinolinol to 5-nitro-8-quinolinol to 8-quinolinol.

Reações de 1,2-dicloro-4,5-dinitrobenzeno com aminas: monossubstituição de nitro e dissubstituição de cloro e nitro

1,2-dichloro-4,5-dinitrobenzene (DCDNB) reacts with primary and secondary amines, in acetonitrile, at room temperature, to give a monosubstituted nitro product with a yield of 85 to 95%. The chloro-nitro-disubstituted product is formed with excess amine under reflux. Piperidine, pyrroline, dimethylamine and methylamine were the most reactive reagents in both mono- and disubstitution.

Síntese de 5-nitro-isatina e 5-cloro-isatina a partir da isonitrosoacetanilida

This article describes the preparation of 5-nitroisatin and of 5-chloroisatin from isonitrosoacetanilide in a single step, using readily available and inexpensive reagents. These reactions require around 90 minutes and may be carried out as an undergraduate experiment, providing an opportunity to discuss the electrophilic aromatic substitution mechanism, as well as spectroscopic techniques for product identification.

Nitro derivatives and other constituents of Aristolochia melastoma

A phytochemical study of Aristolochia melastoma Manso has led to the isolation and identification of 20 known compounds, including aristolochic acids, sodium aristolochates, lignan, flavonoids, and nitro phenylethyl derivatives. Their structures were established by spectroscopic analysis. The presence of thalictricoside and secoisolariciresinol dimethyl ether diacetate is reported for the first time in the Aristolochiaceae family. In addition, the presence of nitro compounds in this species is significant.

Synthesis of 2-azetidinone derivatives of 6-nitro-1H-indazole and their biological importance

A new series of 3-chloro-1-{[2-(6-nitro-1H-indazol-1-yl)ethyl]amino}-4-(substituted phenyl)-2-azetidinones (4a-j) was synthesized in four steps from 6-nitro-1H-indazole and characterized by IR, ¹H NMR, 13C NMR, FAB-mass spectrometry and chemical methods. Compounds 4(a-j) were screened in vitro for their antibacterial, antifungal and antitubercular activities against some selected microorganism and for their antiinflammatory activity (in vivo) against albino rats (either sex). All above activities of compounds 4(a-j) showed acceptable results.

A time-dependent, two-step binding mode of the nitro dye flavianic acid to trypsin in acid media

Synthetic dyes bind to proteins causing selective coprecipitation of the complexes in acid aqueous solution by a process of reversible denaturation that can be used as an alternative method for protein fractionation. The events that occur before precipitation were investigated by equilibrium dialysis using bovine trypsin and flavianic acid as a model able to cause coprecipitation. A two-step mode of interaction was found to be dependent on the incubation periods allowed for binding, with pronounced binding occurring after 42 h of incubation. The first step seems to involve hydration effects and conformational changes induced by binding of the first dye molecule, following rapid denaturation due to the binding of six additional flavianate anions to the macromolecule.

Nitro-fatty acids: novel anti-inflammatory lipid mediators

Nitro-fatty acids are formed and detected in human plasma, cell membranes, and tissue, modulating metabolic as well as inflammatory signaling pathways. Here we discuss the mechanisms of nitro-fatty acid formation as well as their key chemical and biochemical properties. The electrophilic properties of nitro-fatty acids to activate anti-inflammatory signaling pathways are discussed in detail. A critical issue is the influence of nitroarachidonic acid on prostaglandin endoperoxide H synthases, redirecting arachidonic acid metabolism and signaling. We also analyze in vivo data supporting nitro-fatty acids as promising pharmacological tools to prevent inflammatory diseases.

McCoy cell line as a possible model containing CD4+ receptors for the study of HIV-1 replication

Several studies have recently shown the use of recombinant rabies virus as potential vector-viral vaccine for HIV-1. The sequence homology between gp 120 and rabies virus glycoprotein has been reported. The McCoy cell line has therefore been used to show CD4+ or CD4+ like receptors. Samples of HIV-1 were isolated, when plasma of HIV-1 positive patients was inoculated in the McCoy cell line. The virus infection was then studied during successive virus passages. The proteins released in the extra cellular medium were checked for protein activity, by exposure to SDS Electrophoresis and blotting to nitro-cellulose filter, then reacting with sera of HIV positive and negative patients. Successive passages were performed, and showed viral replication, membrane permeabilization, the syncytium formation, and the cellular lysis (cytopathic effect). Flow cytometry analysis shows clear evidence that CD4+ receptors are present in this cell line, which enhances the likelihood of easy isolation and replication of HIV. The results observed allow the use of this cell line as a possible model for isolating HIV, as well as for carrying out studies of the dynamics of viral infection in several situations, including exposure to drugs in pharmacological studies, and possibly studies and analyses of the immune response in vaccine therapies.

Uso prévio do Ro 7-1051 na doença de Chagas experimental em camondongos

No presente estudo camondongos "Swiss" foram submetidos a tratamento com a droga Ro 7-1051 (N-Benzil-2-Nitro-imidazolacetamida) antes de sua inoculação com a cepa Colombiana do T. cruzi e comparados com animais inocuiados com a mesma cepa e tratados em fase inicial de infecção. Com avaliação feita por parasitemia periférica, xenodiagnõstico, sub-inoculação em camondongos recém-nascidos e exame histopatológico foram obtidos melhores resultados com os animais submetidos a tratamento prévio, tendo-se verificado que 55,5% dos animais permaneceram negativados durante o curso da experiência, enquanto os tratados precocemente tiveram um índice de cura de 28,5%.

Alteração da resposta imune mediada por células durante o tratamento com Benzonidazol

Coelhos inoculados com tripomastigotas da cepa Ernestina do Trypanosoma cruzi tiveram parasitemias, demonstradas pelo xenodiagnóstico, até cinco meses e meio após a infecção. O tratamento de alguns desses coelhos com benzonidazol, na dose de 8mg/kg durante sessenta dias, após dois meses de infecção, resultou na negativação dos xenos após 30 dias de uso da medicação. Os coelhos chagásicos crônicos, após seis meses de infecção, já tinham a parasitemia subpatente quando foram submetidos a tratamento idêntico àqueles da fase aguda. Em ambos os casos, os coelhos tratados com benzonidazol tiveram títulos de anticorpos humorais semelhantes àqueles verificados nos coelhos chagásicos não- tratados, inclusive durante a quimioterapia. A não alteração da imunidade humoral em coelhos tratados foi comprovada quando animais chagásicos e não chagásicos submetidos ao tratamento produziram títulos de anticorpos hemolíticos idênticos àqueles verificados nos animais não-tratados. Em acentuado contraste, a função imune timo-dependente foi severamente alterada pelo uso do benzonidazol. As reações de hipersensibilidade tardia contra um antígeno sub- celular do T. cruzi foram suprimidas durante a vigência do tratamento dos coelhos chagásicos. Paralelamente, estas reações eram intensas nos coelhos chagásicos não-tratados e negativas em coelhos controles normais. Todavia, as reações cutâneas tornaram-se novamente positivas 10 dias após o tratamento. Foi interessante notar que as reações de hipersensibilidade tardia in vivo, em coelhos imunizados com BCG e testados com PPD ou em coelhos sensibilizados com DNCB também foram suprimidas durante o tratamento com o benzonidazol. Contudo, as reações de imunidade celular contra estes antígenos também reverteram aos valores normais 7 a 10 dias após a suspensão do benzonidazol. Resultados semelhantes foram relatados em relação ao nifurtimox, outra droga utilizada no tratamento da doença de Chagas. 0 benzonidazol e o nifurtimox são compostos nitro-aromáticos cuja nitrorredução resulta na formação de metabólitos intermediários potencialmente citotóxicos para o protozoário e para as células do hospedeiro.

Differing phagocytic function of monocytes and neutrophils in Chagas' cardiopathy according to the presence or absence of congestive heart failure

We evaluated the in vitro phagocytic function and the production of microbicidal oxygen radicals by monocytes and neutrophils of 9 Chagas' heart disease subjects with heart failure and 9 without the syndrome in comparison with 11 healthy subjects, by assessing phagocytosis of Saccharomyces cerevisiae and NBT reduction by peripheral blood phagocytes. Phagocytic index of monocytes of chagasics without heart failure was significantly 6.7 and 10.6 times lower than those of controls and chagasics with the congestive syndrome, respectively, due to a lesser engagement in phagocytosis and to an inability of these cells to ingest particles. Neutrophils also show in chagasics without heart failure PI 11.2 and 19.8 times lower than that of controls and chagasics with heart failure, respectively. The percent of NBT reduction was normal and similar for the three groups. Balanced opposite effects of cardiovascular and immune disturbances may be acting in Chagas' disease subjects with heart failure paradoxically recovering the altered phagocytic function.