Biomed Res Int. 2014;2014:217269. doi: 10.1155/2014/217269. Epub 2014 Apr 29.

Hyperammonemia associated with valproic acid concentrations.

Vázquez M¹, Fagiolino P¹, Maldonado C¹, Olmos I¹, Ibarra M¹, Alvariza S¹, Guevara N¹, Magallanes L¹, Olano I².

Author information

1: Pharmaceutical Sciences Department, Faculty of Chemistry, Universidad de la República, Avenida General Flores 2124, P.O. Box 1157, 11800 Montevideo, Uruguay ; Therapeutic Drug Monitoring Service, "Dr. Manuel Quintela" Clinical Hospital, Universidad de la República, Avenida Italia s/n, 11609 Montevideo, Uruguay.
2: "Sanatorio Canzani" Hospital, Banco de Previsión Social, Martín García 1363, 11800 Montevideo, Uruguay.

Abstract

Valproic acid, a branched short-chain fatty acid, has numerous action mechanisms which turn it into a broad spectrum anticonvulsant drug and make its use possible in some other pathologies such as bipolar disorder. It is extensively metabolized in liver, representing β -oxidation in the mitochondria one of its main metabolic route (40%). Carnitine is responsible for its entry into the mitochondria as any other fatty acid. Long-term high-dose VPA therapy or acute VPA overdose induces carnitine depletion, resulting in high levels of ammonia in blood. As a high correlation between salivary valproic acid levels and plasma ultrafiltrate levels was found in humans, saliva becomes a promising monitoring fluid in order to study valproic acid pharmacokinetics and its toxic effect. Extended-release (twice daily) formulations of valproic acid or carnitine supplementation are the proposed two therapeutic strategies in order to reverse hyperammonemia.