Por favor, use este identificador para citar o enlazar este ítem: http://repositorio.ufc.br/handle/riufc/5088
Tipo: Artigo de Periódico
Título : Antinociceptive effects of interleukin-4, -10, and -13 on the writhing response in mice and zymosan-induced knee joint incapacitation in rats
Autor : Vale, Mariana L.
Marques, Jaciara B.
Moreira, Camila A.
Rocha, Francisco Aírton C.
Ferreira, Sérgio H.
Poole, Stephen
Cunha, Fernando Q.
Ribeiro, Ronaldo A.
Palabras clave : Interleucina-4;Interleucina-10;Interleucina-13;Articulação do Joelho
Fecha de publicación : ene-2003
Editorial : The Journal of Pharmacology and Experimental Therapeutics
Citación : VALE, M. L. et al. Antinociceptive effects of interleukin-4, -10, and -13 on the writhing response in mice and zymosan-induced knee joint incapacitation in rats. The Journal of Pharmacology and Experimental Therapeutics, Rockville Pike Bethesda, Maryland, v. 304, n. 1, p. 102-108, jan. 2003.
Abstract: The antinociceptive effects of interleukin (IL)-4, -10, and -13 were investigated in two different experimental pain models. Our results showed that pretreatment (30 min) with IL-4 (1–5 ng/animal), IL-10 (0.4–10 ng/animal), or IL-13 (0.4 –2.5 ng/animal) inhibited the writhing response induced by the i.p. administration of acetic acid (53–89%) or zymosan (63–74%) in mice, and the knee joint incapacitation induced by i.a. injection of zymosan (49–66%) in rats. Neither of the cytokines affected the pain elicited in mice using the hot-plate test. This analgesic effect of IL-4, -10, and -13 was not reversed by the combined pretreatment with the opioid receptor antagonist naloxone. IL-4, -10, or -13 significantly inhibited the release of both tumor necrosis factor (TNF)- (60, 53, and 100%, respectively) and IL-1 (80, 100, and 100%, respectively) by mice peritoneal macrophages obtained after local (i.p.) injection of zymosan. Antisera against IL-4, -10, and -13 potentiated both the zymosan- induced writhing response and the articular incapacitation. Our results demonstrate that IL-4, -10, and -13 display analgesic activity that is probably not due to endogenous opioid release. This analgesic effect could be related to a peripheral mechanism, probably via the inhibition of the release of the pro-inflammatory cytokines TNF- and IL-1 by resident peritoneal macrophages.
URI : http://www.repositorio.ufc.br/handle/riufc/5088
ISSN : 0022-3563
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