Δ2-Valproate biotransformation using human liver microsomal fractions

Abstract

The metabolism of 2-n-propyl-2-pentenoate (Δ²-VPA) was evaluated in human hepatic microsomal fractions. Two biotransformation pathways have been particularly investigated. In the presence of the cytochrome P-450 co-factor, NADPH, the main metabolites recovered were Δ³-VPA, Δ^2,4-VPA and VPA. The glucuronidation of Δ²-VPA was also studied on various hepatic microsomal fractions using Brij^® 35 as activator and UDP-glucuronic acid as co-factor. A large interindividual variability occurred in this metabolic pathway.K _m andV _max were 0.85 mmol/l and 1.75 nmol·min⁻¹·mg⁻¹, respectively, for Δ²-VPA and 1.11 mmol/l and 5.71 nmol·min⁻¹·mg⁻¹ for VPA, respectively. The good correlationr=0.82; p2-VPA as well as the mutual inhibition of each other's glucuronidation strongly suggests that (a) common single UDP-glucuronosyltransferase isoenzyme(s) was (were) involved in this glucuronidation step. The glucuronidation of specific substrates for various UDP-glucuronosyltransferase isoenzymes showed a good relationship between the glucuronidations of Δ²-VPA and morphine, a substrate for UDP-glucuronosyltransferase-2B. Moreover, morphine competitively inhibits A -VPA glucuronidation. It seems the same isoenzyme or, at least, (a) very closely related isoenzyme(s) belonging to UDP-glucuronosyltransferase-2 isoenzyme, is involved in Δ²-VPA glucuronidation.