Anticonvulsant Activity of Phenytoin-lipid Conjugates, a New Class of Phenytoin Prodrugs

Author:

Scriba Gerhard K E1,Lambert Didier M21,Poupaert Jacques H21

Affiliation:

1. Department of Pharmaceutical Chemistry, School of Pharmacy, University of Münster, Hittorfstrasse 58-62, 48149 Münster, Germany

2. Laboratory of Medicinal Chemistry, School of Pharmacy, Catholic University of Louvain, CMFA 73.40, Avenue E. Mounier 73, 1200 Brussels, Belgium

Abstract

Abstract The anticonvulsant activity of phenytoin-lipid conjugates obtained by covalent binding of 3-hydroxy-methylphenytoin to dimyristoylglycerides via a succinidyl linkage, to 2-(1,3-dimyristoylglyceryl)butyric acid and to 3-myristoyl-2-myristoylmethylpropionic acid was evaluated in the maximal electroshock (MES) test and the seizure threshold test with subcutaneous pentetrazol. The phenytoin-lipid conjugates were less active than the parent drug in the MES test after intraperitoneal administration as suspensions, but exhibited comparable activity when injected as a solution in dimethysulphoxide. They also protected mice from MES-induced seizures following oral administration of aqueous suspensions of the compounds or when incorporated into emulsions. The anticonvulsant activity could be correlated to in-vitro pancreatic lipase-mediated hydrolysis. The bis-deacyl derivatives were at least as active but in some cases also more toxic than phenytoin. Oral administration of two of the lipid conjugates resulted in a faster onset of the anticonvulsant activity compared with the administration of an equimolar dose of phenytoin itself. All compounds were inactive in the subcutaneous pentetrazol test. It is concluded that the lipids act as prodrugs of phenytoin, which is generated by lipolysis upon oral administration.

Publisher

Oxford University Press (OUP)

Subject

Pharmaceutical Science,Pharmacology

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