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DOI: 10.1055/s-2008-1071456
© Georg Thieme Verlag KG Stuttgart · New York
L-Carnitine Replacement Therapy in Chronic Valproate Treatment
Publication History
Publication Date:
19 March 2008 (online)
Abstract
Ten epileptic children with chronic valproic acid (VPA) treatment were given L-carnitine for 14 days. As compared to age and sex matched control subjects the carnitine status of the VPA treated children showed carnitine insufficiency prior to the carnitine administration with lower total and free carnitine in plasma and in urine. In response to the extra intake the plasma free and esterified carnitines increased 1.7-fold. The daily excreted amount of esterified carnitines increased 6.5-fold (1.55±0.23 vs 10.1±1.68µmol/kg/day, means ±SEM, p<0.005) showing that a considerable part of the administered carnitine participated in the elimination of acyl groups from the body. The depressed level of β-hydroxybutyrate in the plasma (31.8 ±7.42 vs controls 118.0±16.0 µmol/1, means ±SEM, p<0.005) remained unaffected by the carnitine administration (29.7±7.06 µmol/1) suggesting that the hypoketonemia is not a direct consequence of the carnitine insufficiency. No differences were observed in the plasma level of free fatty acids, triglycerides and in insulin: glucagon ratios between the VPA treated and control subjects, suggesting that lipolysis of fats and the hepatic hormonal control mediated by these hormones are not the sites at which VPA causes reduced fasting ketogenesis. The plasma level of VPA and the seizure control remained unaffected by carnitine treatment.
Key words
Carnitine - Valproic acid - Ketone bodies - Fat oxidation