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J Vet Sci. 2009 Mar;10(1):15-22 DOI: 10.4142/jvs.2009.10.1.15 |
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Effects of L-NAME, a non-specific nitric oxide synthase inhibitor, on
AlCl3-induced toxicity in the rat forebrain cortex
Ivana D. Stevanovi?1,*, Marina D. Jovanovi?1, Ankica Jelenkovi?2, Miodrag ?oli?1, Ivana Stojanovi?3, Milica Ninkovi?1 |
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1Military Medical Academy, Institute for Medical Research, Crnotravska 17, Belgrade, Serbia
2Institute for Biological Research, Belgrade, Serbia
3Department of Biochemistry, Faculty of Medicine, University of Ni?, Ni?, Serbia
* ivanav13@yahoo.ca |
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The present experiments were done to determine the
effectiveness of a non-specific nitric oxide synthase inhibitor,
N-nitro-L-arginine methyl ester (L-NAME), on oxidative
stress parameters induced by aluminium chloride (AlCl3)
intrahippocampal injections in Wistar rats. Animals were
sacrificed 3 h and 30 d after treatments, heads were
immediately frozen in liquid nitrogen and forebrain cortices
were removed. Crude mitochondrial fraction preparations
of forebrain cortices were used for the biochemical analyses:
nitrite levels, superoxide production, malondialdehyde
concentrations, superoxide dismutase (SOD) activities and
reduced glutathione contents. AlCl3 injection resulted in
increased nitrite concentrations, superoxide anion production,
malondialdehyde concentrations and reduced glutathione
contents in the forebrain cortex, suggesting that AlCl3
exposure promoted oxidative stress in this brain structure.
The biochemical changes observed in neuronal tissues showed
that aluminium acted as a pro-oxidant. However, the nonspecific
nitric oxide synthase (NOS) inhibitor, L- NAME,
exerted anti-oxidant actions in AlCl3-treated animals. These
results revealed that NO-mediated neurotoxicity due to
intrahippocampal AlCl3 injection spread temporally and
spatially to the forebrain cortex, and suggested a potentially
neuroprotective effect for L-NAME.
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