Beer consumption reduces cerebral oxidation caused by aluminum toxicity by normalizing gene expression of tumor necrotic factor alpha and several antioxidant enzymes

Aluminum (Al)-induced neurotoxicity is well known and different salts of aluminum have been reported to accelerate oxidative damage to biomolecules. The present study has examined whether silicon consumed in the form of silicic acid or beer could potentially inhibit aluminum toxicity in the brain. M...

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Bibliographic Details
Published in:Food and chemical toxicology 2008-03, Vol.46 (3), p.1111-1118
Main Authors: Gonzalez-Muñoz, M.J., Meseguer, I., Sanchez-Reus, M.I., Schultz, A., Olivero, R., Benedí, J., Sánchez-Muniz, F.J.
Format: Article
Language:English
Subjects:
Alcoholism and acute alcohol poisoning
Aluminum
Aluminum - toxicity
animal models
Animals
antioxidant activity
Antioxidant enzymes
antioxidants
Base Sequence
Beer
beers
Biological and medical sciences
Brain
Brain - drug effects
Brain - metabolism
Chemical and industrial products toxicology. Toxic occupational diseases
DNA Primers
enzymes
Enzymes - genetics
gene expression
Gene Expression - drug effects
lipid peroxidation
Male
Medical sciences
messenger RNA
Metals and various inorganic compounds
Mice
neurotoxicity
oxidation
silicic acid
Silicon
Thiobarbituric Acid Reactive Substances - metabolism
TNFα
Toxicology
tumor necrosis factor-alpha
Tumor Necrosis Factor-alpha - genetics
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Summary:Aluminum (Al)-induced neurotoxicity is well known and different salts of aluminum have been reported to accelerate oxidative damage to biomolecules. The present study has examined whether silicon consumed in the form of silicic acid or beer could potentially inhibit aluminum toxicity in the brain. Male mice were administered with Al(NO 3) 3 orally at a dose of 450 mg/kg/day in drinking water for 3 month. Experimental mice were given Al(NO 3) 3 along with 50 mg/L of silicic acid or with 0.5 ml/day of beer. Al brain levels in the Al group were four times higher than those of control mice while silicic acid and beer group values were 40% lower than those of the Al group. We have observed that beer prevented accumulation of lipid damage significantly, which resulted from aluminum intake. Decline in the expression of mRNA of endogenous antioxidant enzymes associated with aluminum administration was also inhibited by beer and silicic acid. The tumor necrosis factor alpha (TNFα) RNA expression was normalized in silicic acid and beer groups. Very high and significant correlations were found for the different parameters tested suggesting that moderate consumption of beer, due to its silicon content, effectively protects against the neurotoxic effects of aluminum.
ISSN:0278-6915
1873-6351
DOI:10.1016/j.fct.2007.11.006