Pharmacokinetics and Anticonvulsant Activity of Three Monoesteric Prodrugs of Valproic Acid

Khalil Badir; Abdulla Haj-Yehia; Tom B. Vree; Eppo van der Kleijn; Meir Bialer

doi:10.1023/A:1015854118110

Pharmacokinetics and Anticonvulsant Activity of Three Monoesteric Prodrugs of Valproic Acid

Khalil Badir^*, Abdulla Haj-Yehia, Tom B. Vree, Eppo van der Kleijn, Meir Bialer

^*Corresponding author for this work

School of Pharmacy

Research output: Contribution to journal › Article › peer-review

16 Scopus citations

Abstract

The pharmacokinetics of valproic acid (VPA) were compared in dogs with those of the prodrugs ethyl valproate (E-VPA), trichloroethyl valproate (T-VPA), and valproyl valproate (V-VPA). Valproic acid, E-VPA, T-VPA, and V-VPA were administered intravenously and orally to six dogs at equimolar doses. The three VPA prodrugs were rapidly converted to VPA. The biotransformation was complete in the case of E-VPA and T-VPA but was only partial in the case of V-VPA. Because of the rapid conversion to the parent drug, after administration of the prodrugs, VPA plasma levels did not yield a sustained-release profile. Further, the anticonvulsant activity of prodrugs was compared in mice to that of VPA and valpromide (VPD). The anticonvulsant activity of E-VPA, T-VPA, and V-VPA was less than that of VPA.

Original language	English
Pages (from-to)	750-753
Number of pages	4
Journal	Pharmaceutical Research
Volume	8
Issue number	6
DOIs	https://doi.org/10.1023/A:1015854118110
State	Published - Jun 1991

Keywords

esteric prodrugs
pharmacokinetics
valproic acid

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title = "Pharmacokinetics and Anticonvulsant Activity of Three Monoesteric Prodrugs of Valproic Acid",

abstract = "The pharmacokinetics of valproic acid (VPA) were compared in dogs with those of the prodrugs ethyl valproate (E-VPA), trichloroethyl valproate (T-VPA), and valproyl valproate (V-VPA). Valproic acid, E-VPA, T-VPA, and V-VPA were administered intravenously and orally to six dogs at equimolar doses. The three VPA prodrugs were rapidly converted to VPA. The biotransformation was complete in the case of E-VPA and T-VPA but was only partial in the case of V-VPA. Because of the rapid conversion to the parent drug, after administration of the prodrugs, VPA plasma levels did not yield a sustained-release profile. Further, the anticonvulsant activity of prodrugs was compared in mice to that of VPA and valpromide (VPD). The anticonvulsant activity of E-VPA, T-VPA, and V-VPA was less than that of VPA.",

keywords = "esteric prodrugs, pharmacokinetics, valproic acid",

author = "Khalil Badir and Abdulla Haj-Yehia and Vree, {Tom B.} and {van der Kleijn}, Eppo and Meir Bialer",

year = "1991",

month = jun,

doi = "10.1023/A:1015854118110",

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AU - Badir, Khalil

AU - Haj-Yehia, Abdulla

AU - Vree, Tom B.

AU - van der Kleijn, Eppo

AU - Bialer, Meir

PY - 1991/6

Y1 - 1991/6

N2 - The pharmacokinetics of valproic acid (VPA) were compared in dogs with those of the prodrugs ethyl valproate (E-VPA), trichloroethyl valproate (T-VPA), and valproyl valproate (V-VPA). Valproic acid, E-VPA, T-VPA, and V-VPA were administered intravenously and orally to six dogs at equimolar doses. The three VPA prodrugs were rapidly converted to VPA. The biotransformation was complete in the case of E-VPA and T-VPA but was only partial in the case of V-VPA. Because of the rapid conversion to the parent drug, after administration of the prodrugs, VPA plasma levels did not yield a sustained-release profile. Further, the anticonvulsant activity of prodrugs was compared in mice to that of VPA and valpromide (VPD). The anticonvulsant activity of E-VPA, T-VPA, and V-VPA was less than that of VPA.

AB - The pharmacokinetics of valproic acid (VPA) were compared in dogs with those of the prodrugs ethyl valproate (E-VPA), trichloroethyl valproate (T-VPA), and valproyl valproate (V-VPA). Valproic acid, E-VPA, T-VPA, and V-VPA were administered intravenously and orally to six dogs at equimolar doses. The three VPA prodrugs were rapidly converted to VPA. The biotransformation was complete in the case of E-VPA and T-VPA but was only partial in the case of V-VPA. Because of the rapid conversion to the parent drug, after administration of the prodrugs, VPA plasma levels did not yield a sustained-release profile. Further, the anticonvulsant activity of prodrugs was compared in mice to that of VPA and valpromide (VPD). The anticonvulsant activity of E-VPA, T-VPA, and V-VPA was less than that of VPA.

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KW - pharmacokinetics

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Pharmacokinetics and Anticonvulsant Activity of Three Monoesteric Prodrugs of Valproic Acid

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Keywords

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