In Vitro Evaluation of Potential Drug Interactions With Levetiracetam, A New Antiepileptic Agent

In Vitro Evaluation of Potential Drug Interactions With Levetiracetam, A New Antiepileptic Agent

Levetiracetam and its carboxylic metabolite (AcL) were tested for their potential inhibitory effect on 11 different drug metabolizing enzyme activities using human liver microsomes. The following specific assays were investigated: testosterone 6β-hydroxylation [cytochrome P-450 3A4 (CYP3A4)], couma...

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Bibliographic Details
Published in:Drug metabolism and disposition Vol. 27; no. 2; pp. 250 - 254
Main Authors: NICOLAS, J.-M, COLLART, P, GERIN, B, MATHER, G, TRAGER, W, LEVY, R, ROBA, J
Format: Journal Article
Language:English
Published: Bethesda, MD American Society for Pharmacology and Experimental Therapeutics 01-02-1999
Subjects:
Animals
Anticonvulsants - metabolism
Anticonvulsants - pharmacology
Anticonvulsants. Antiepileptics. Antiparkinson agents
Biological and medical sciences
Biomarkers
Butyrates - pharmacology
Cytochrome P-450 Enzyme Inhibitors
Drug Interactions
Enzyme Inhibitors - metabolism
Enzyme Inhibitors - pharmacology
Epoxide Hydrolases - antagonists & inhibitors
Glucuronosyltransferase - antagonists & inhibitors
Humans
In Vitro Techniques
Liver - cytology
Liver - drug effects
Liver - metabolism
Male
Medical sciences
Microsomes, Liver - drug effects
Microsomes, Liver - metabolism
Neuropharmacology
Pharmacology. Drug treatments
Piracetam - analogs & derivatives
Piracetam - metabolism
Piracetam - pharmacology
Pyrrolidinones - pharmacology
Rats
Rats, Sprague-Dawley
Rat
Isozyme
Metabolite
Liver
Glycosyltransferases
Anticonvulsant
Epoxide hydrolase
Enzymatic activity
Inhibition
Human
UDP-glucuronosyltransferase
Digestive system
Enzyme
Induction
Transferases
Cytochrome P450
Rodentia
In vitro
Vertebrata
Mammalia
Animal
Ether hydrolases
Hydrolases
Hexosyltransferases
Levetiracetam
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Summary:Levetiracetam and its carboxylic metabolite (AcL) were tested for their potential inhibitory effect on 11 different drug metabolizing enzyme activities using human liver microsomes. The following specific assays were investigated: testosterone 6β-hydroxylation [cytochrome P-450 3A4 (CYP3A4)], coumarin hydroxylation (CYP2A6), ( R )-warfarin hydroxylation (CYP1A2), ( S )-mephenytoin hydroxylation (CYP2C19), p -nitrophenol hydroxylation (CYP2E1) tolbutamide hydroxylation (CYP2C9), dextromethorphan O -demethylation (CYP2D6), epoxide hydrolase and UDP-glucuronyltransferase (UGT) toward paracetamol (UGT1*6), ethinyloestradiol (UGT1*1), p -nitrophenol (UGT(pl 6.2)), and valproic acid. None of these activities were affected by levetiracetam or AcL added at concentrations up to 1 mM. Additionally, primary cultures of rat hepatocytes were used to assess a potential inducing effect of levetiracetam on CYPs. Phenobarbital (2 mM), β-naphtoflavone (40 μM), dexamethasone (1 μM), and phenytoin (up to 300 μM) were tested as positive controls. When added to cells for 48 h, all the positive controls increased 7-ethoxycoumarin O -deethylase activity demonstrating the inducibility of CYPs in the present culture conditions. By contrast, levetiracetam did not affect the activity up to 1 mM. The highest levetiracetam concentrations examined in the above in vitro studies are well in excess of those measured in the plasma of patients receiving therapeutic doses. It is thus concluded that levetiracetam is unlikely to produce pharmacokinetic interactions through inhibition of CYPs, UGTs, and epoxide hydrolase. Furthermore, based on the in vitro assays with rat hepatocytes, it could be speculated that levetiracetam does not act as a CYP inducer.
ISSN:0090-9556
1521-009X