Inflammatory oedema induced by Lachesis muta muta (Surucucu) venom and LmTX-I in the rat paw and dorsal skin

FERREIRA, TATIANECAMARGO, ENILTON A.RIBELA, MARIA T.C.P.DAMICO, DANIELA C.MARANGONI, SERGIOANTUNES, EDSONNUCCI, GILBERTO deLANDUCCI, ELEN C.T.2014-07-152014-07-302014-07-152014-07-302009FERREIRA, TATIANE; CAMARGO, ENILTON A.; RIBELA, MARIA T.C.P.; DAMICO, DANIELA C.; MARANGONI, SERGIO; ANTUNES, EDSON; NUCCI, GILBERTO de; LANDUCCI, ELEN C.T. Inflammatory oedema induced by Lachesis muta muta (Surucucu) venom and LmTX-I in the rat paw and dorsal skin. <b>Toxicon</b>, v. 53, n. 1, p. 69-77, 2009. DOI: <a href="https://dx.doi.org/10.1016/j.toxicon.2008.10.016">10.1016/j.toxicon.2008.10.016</a>. Disponível em: http://repositorio.ipen.br/handle/123456789/4857.0041-0101http://repositorio.ipen.br/handle/123456789/4857The ability of crude venom and a basic phospholipase A2 (LmTX-I) from Lachesis muta muta venom to increase the microvascular permeability in rat paw and skin was investigated. Crude venom or LmTX-I were injected subplantarly or intradermally and rat paw oedema and dorsal skin plasma extravasation were measured. Histamine release from rat peritoneal mast cell was also assessed. Crude venom or LmTX-I induced dose-dependent rat paw oedema and dorsal skin plasma extravasation. Venom-induced plasma extravasation was inhibited by the histamine H1 antagonist mepyramine (6 mg/kg), histamine/5-hydroxytriptamine antagonist cyproheptadine (2 mg/kg), cyclooxygenase inhibitor indomethacin (5 mg/kg), nitric oxide synthesis inhibitor l-NAME (100 nmol/site), tachykinin NK1 antagonist SR140333 (1 nmol/site) and bradykinin B2 receptor antagonist Icatibant (0.6 mg/kg). Platelet-activating factor (PAF) antagonist PCA4248 (5 mg/kg) had no effect. LmTX-I-induced skin extravasation was inhibited by cyproheptadine, mepyramine, indomethacin and PCA4248, while l-NAME and SR140333 had no effect. Additionally, both Lachesis muta muta venom and LmTX-I concentration-dependently induced histamine release from rat mast cells. In conclusion, Lachesis muta muta venom and LmTX-I increase microvascular permeability by mechanisms involving in vivo mast cell activation and arachidonic acid metabolites. Additionally, crude venom-induced responses also involve substance P, nitric oxide and bradykinin release, whether LmTX-I-induced responses involve PAF.69-77openAccesssnakesvenomsvascular diseasesinflammationpermeabilitymast cellsratsskin effectInflammatory oedema induced by Lachesis muta muta (Surucucu) venom and LmTX-I in the rat paw and dorsal skinArtigo de periódico15310.1016/j.toxicon.2008.10.016