972 resultados para secretory phospholipase A2
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Snake venom metalloproteinases (SVMPs) participate in a number of important biological, physiological and pathophysiological processes and are primarily responsible for the local tissue damage characteristic of viperid snake envenomations. The use of medicinal plant extracts as antidotes against animal venoms is an old practice, especially against snake envenomations. Such plants are sources of many pharmacologically active compounds and have been shown to antagonize the effects of some venoms and toxins. The present study explores the activity of triacontyl p-coumarate (PCT), an active compound isolated from root bark of Bombacopsis glabra vegetal extract (Bg), against harmful effects of Bothropoides pauloensis snake venom and isolated toxins (SVMPs or phospholipase A2). Before inhibition assays, Bg or PCT was incubated with venom or toxins at ratios of 1:1 and 1:5 (w/w; venom or isolated toxins/PCT) for 30 min at 37 °C. Treatment conditions were also assayed to simulate snakebite with PCT inoculated at either the same venom or toxin site. PCT neutralized fibrinogenolytic activity and plasmatic fibrinogen depletion induced by B. pauloensis venom or isolated toxin. PCT also efficiently inhibited the hemorrhagic (3MDH-minimum hemorrhagic dose injected i.d into mice) and myotoxic activities induced by Jararhagin, a metalloproteinase from B. jararaca at 1:5 ratio (toxin: inhibitor, w/w) when it was previously incubated with PCT and injected into mice or when PCT was administered after toxin injection. Docking simulations using data on a metalloproteinase (Neuwiedase) structure suggest that the binding between the protein and the inhibitor occurs mainly in the active site region causing blockade of the enzymatic reaction by displacement of catalytic water. Steric hindrance may also play a role in the mechanism since the PCT hydrophobic tail was found to interact with the loop associated with substrate anchorage. Thus, PCT may provide a alternative to complement ophidian envenomation treatments. © 2012 Elsevier Ltd. All rights reserved.
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The mortality caused by snakebites is more damaging than many tropical diseases, such as dengue haemorrhagic fever, cholera, leishmaniasis, schistosomiasis and Chagas disease. For this reason, snakebite envenoming adversely affects health services of tropical and subtropical countries and is recognized as a neglected disease by the World Health Organization. One of the main components of snake venoms is the Lys49-phospholipases A2, which is catalytically inactive but possesses other toxic and pharmacological activities. Preliminary studies with MjTX-I from Bothrops moojeni snake venom revealed intriguing new structural and functional characteristics compared to other bothropic Lys49-PLA2s. We present in this article a comprehensive study with MjTX-I using several techniques, including crystallography, small angle X-ray scattering, analytical size-exclusion chromatography, dynamic light scattering, myographic studies, bioinformatics and molecular phylogenetic analyses.Based in all these experiments we demonstrated that MjTX-I is probably a unique Lys49-PLA2, which may adopt different oligomeric forms depending on the physical-chemical environment. Furthermore, we showed that its myotoxic activity is dramatically low compared to other Lys49-PLA2s, probably due to the novel oligomeric conformations and important mutations in the C-terminal region of the protein. The phylogenetic analysis also showed that this toxin is clearly distinct from other bothropic Lys49-PLA2s, in conformity with the peculiar oligomeric characteristics of MjTX-I and possible emergence of new functionalities inresponse to environmental changes and adaptation to new preys. © 2013 Salvador et al.
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Coordenação de Aperfeiçoamento de Pessoal de Nível Superior (CAPES)
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Coordenação de Aperfeiçoamento de Pessoal de Nível Superior (CAPES)
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Conselho Nacional de Desenvolvimento Científico e Tecnológico (CNPq)
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Coordenação de Aperfeiçoamento de Pessoal de Nível Superior (CAPES)
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Pós-graduação em Ciências Biológicas (Genética) - IBB
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Este estudo investigou a toxicidade aguda oral, o efeito antinociceptivo em modelos de nocicepção química e térmica, bem como a atividade anti-inflamatória em modelos de carragenina e óleo de cróton do extrato hidroetanólico de partes aéreas de Portulaca pilosa (EHEPp). Identificou também alguns possíveis mecanismos envolvidos na antinocicepção do extrato, além dos seus efeitos sobre o sistema nervoso central de ratos. No teste de toxicidade aguda oral, o tratamento com EHEPp (2000 mg/kg) não causou óbitos. No teste de contorções abdominais induzidas por ácido acético, o EHEPp (100, 200, 400 e 600 mg/kg), por via oral (v.o.), reduziu significantemente o número de contorções em 18.18, 33.25, 47.27, 65.81 e 73.94%, respectivamente. No teste da placa quente, o tratamento com EHEPp (200, 400 e 600 mg/kg, v.o.) não alterou a latência ao estímulo térmico de 50 ± 0,5 ºC. No teste da formalina, o tratamento com EHEPp (200,400 e 600mg/kg, v.o.) reduziu de maneira significativa o tempo de lambida nas fases neurogênica (1ª fase) em 38.79, 60.61 e 75.18 %, e inflamatória (2ª fase) em 49.23, 53.03 e 87.53 %, respectivamente. A administração prévia de naloxona reverteu, significativamente, o efeito do EHEPp (600 mg/kg, v.o.) em ambas as fases do teste da formalina. O pré-tratamento com o L-NAME e azul de metileno reverteu o efeito do EHEPp (600 mg/kg, v.o.) de maneira significante em ambas as fases do teste da formalina. O pré-tratamento com o fármaco glibenclamida também reverteu de maneira significativa o efeito do EHEPp (600 mg/kg, v.o.) em ambas as fases do teste da formalina. O EHEPp, na dose 600 mg/kg, v.o., não afetou a atividade locomotora dos ratos submetidos ao teste do campo aberto. No teste de edema de pata induzido por carragenina e edema de orelha induzido pelo óleo cróton, o EHEPp (400 e 600 mg/kg, v.o.) não inibiu a formação de edema de maneira significante em ambos os testes. Os resultados deste estudo mostraram que o HEEPp, oralmente, apresentou baixa toxicidade e sua atuação antinociceptiva observada na fase neurogênica pode envolver interações periféricas com receptores opióides e ativação da via NO/GCs/GMPc/ KATP. Já a atividade antinociceptiva observada na fase inflamatória parece não depender de inibição da via bioquímica fosfolipase A2/ciclo-oxigenases, mas de interações periféricas com receptores opióides e com a via NO/GCs/GMPc/KATP.
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Coordenação de Aperfeiçoamento de Pessoal de Nível Superior (CAPES)
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This research presents a study of structural complexes formed between the bothropstoxin BthTX-I and PrTX-I and phospholipase A2 (PLA2s) inhibitor 12- methoxy-4-methyl-voachalotine (MMV) of Tabernamontana catharinensis and rosmarinic acid (Cv-RA) of Rosmarinus officinalis. For both were used cocrystallization experiments with the toxins and inhibitors. In the future, the experimental three-dimensional structures of these complexes will be obtained through the technique of crystallography. Simultaneously, construction occurred in silico of inhibitors Cv-RA and MMV and attempts of docking between these binders and protein structures. These theoretical data provide important information regarding the nature of interactions between inhibitors, toxins and structural changes induced by the protein molecule inhibitors. Therefore, the acquisition of this information has great value to identification, characterization and development (drug design) of compounds with great potential for biotechnology and drug use. Considering further and more relevant aplications, these compounds could be used to control symptoms in many cases of ophidic poisoning and also in combating of pathological processes (degenerative inflammatory diseases and auto-immune diseases, Alzheimer's disease, schizophrenia, among others) whose causes are related to molecules belonging to the same groups of proteins which are classified bothropstoxin that were studied in this project
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Renal alterations caused by Bothrops venom and its compounds are studied to understand these effects and provide the best treatment. Previously, we studied the renal effect of the whole venom of Bothrops marajoensis and its phospholipase A2 (PLA2), but these effects could not to be attributed to PLA2. To continue the study, we report in this short communication the effects of l-amino acid oxidase from B. marajoensis venom (LAAOBm) on renal function parameter alterations observed in the same model of isolated perfused kidney, as well as the cytotoxic effect on renal cells. LAAOBm caused a decrease in PP, RVR, UF, GFR, %TNa(+) and %TCl(-), very similar to the effects of whole venom using the same model. We also demonstrated its cytotoxicity in MDCK cells with IC50 of 2.5 μg/mL and late apoptotic involvement demonstrated by flow cytometry assays. In conclusion, we suggested that LAAOBm is a nephrotoxic compound of B. marajoensis venom.
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Coordenação de Aperfeiçoamento de Pessoal de Nível Superior (CAPES)
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Coordenação de Aperfeiçoamento de Pessoal de Nível Superior (CAPES)
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Conselho Nacional de Desenvolvimento Científico e Tecnológico (CNPq)
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Conselho Nacional de Desenvolvimento Científico e Tecnológico (CNPq)
