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Título
Inhibition of neuronal nitric oxide synthase activity by N1‐acetyl‐5‐methoxykynuramine, a brain metabolite of melatonin
Autor
Año del Documento
2006
Descripción
Producción Científica
Documento Fuente
Journal of Neurochemistry, Septiembre 2006, vol. 98, n. 6, p. 2023-2033
Abstract
We assessed the effects of melatonin, N(1)-acetyl-N (2)-formyl-5-methoxykynuramine (AFMK) and N(1)-acetyl-5-methoxykynuramine (AMK) on neuronal nitric oxide synthase (nNOS) activity in vitro and in rat striatum in vivo. Melatonin and AMK (10(-11)-10(-3) m), but not AFMK, inhibited nNOS activity in vitro in a dose-response manner. The IC(50) value for AMK (70 microm) was significantly lower than for melatonin (>1 mm). A 20% nNOS inhibition was reached with either 10(-9) m melatonin or 10(-11) m AMK. AMK inhibits nNOS by a non-competitive mechanism through its binding to Ca(2+)-calmodulin (CaCaM). The inhibition of nNOS elicited by melatonin, but not by AMK, was blocked with 0.05 mm norharmane, an indoleamine-2,3-dioxygenase inhibitor. In vivo, the potency of AMK to inhibit nNOS activity was higher than that of melatonin, as a 25% reduction in rat striatal nNOS activity was found after the administration of either 10 mg/kg of AMK or 20 mg/kg of melatonin. Also, in vivo, the administration of norharmane blocked the inhibition of nNOS produced by melatonin administration, but not the inhibition produced by AMK. These data reveal that AMK rather than melatonin is the active metabolite against nNOS, which may be inhibited by physiological levels of AMK in the rat striatum.
ISSN
0022-3042
Revisión por pares
SI
Patrocinador
This work was supported in part by the Instituto de Salud Carlos III (ISCIII, Spain) through grants PI02-1447, PI03-0817, PI02-1181, SAF02-01688 and G03/137. JL has a ‘Contrato de Investigadores’ (ISCIII, Spain); MIR and VT are predoctoral fellows from ISCIII, and LCL is a postdoctoral fellow from the Ministerio de Educacio´n
(Spain).
Idioma
eng
Tipo de versión
info:eu-repo/semantics/publishedVersion
Derechos
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