Influence of verapamil on the efflux and metabolism of 14C moxidectin in cultured rat hepatocytes

Influence of verapamil on the efflux and metabolism of 14C moxidectin in cultured rat hepatocytes

Moxidectin (MOX) is an antiparasitic drug widely used in cattle, sheep and companion animals. As a result of the implication of cytochrome P450 3 A in the metabolism of MOX and the role of competitor substrates of P‐glycoprotein (Pgp) in modification of the bioavailability of endectocides, we studie...

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Bibliographic Details
Published in:Journal of veterinary pharmacology and therapeutics Vol. 24; no. 3; pp. 171 - 177
Main Authors: Dupuy, J., Larrieu, G., Sutra, J. F., Eeckhoutte, C., Alvinerie, M.
Format: Journal Article
Language:English
Published: Oxford UK Blackwell Science Ltd 01-06-2001
Subjects:
Animals
Anthelmintics - pharmacokinetics
Anti-Bacterial Agents - pharmacokinetics
Area Under Curve
ATP-Binding Cassette, Sub-Family B, Member 1 - metabolism
Carbon Radioisotopes - pharmacokinetics
Drug Interactions
Hepatocytes - metabolism
Macrolides
Male
Microsomes, Liver - metabolism
Rats
Rats, Sprague-Dawley
Verapamil - pharmacology
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Summary:Moxidectin (MOX) is an antiparasitic drug widely used in cattle, sheep and companion animals. As a result of the implication of cytochrome P450 3 A in the metabolism of MOX and the role of competitor substrates of P‐glycoprotein (Pgp) in modification of the bioavailability of endectocides, we studied the influence of verapamil (a multidrug‐resistance reversing agent) on the metabolism of 14C moxidectin in cultured rat hepatocytes over 72 h. The metabolism of MOX remained low: 10.79 ± 1.99% of the total 14C moxidectin for the main detected metabolite in verapamil‐treated cells and 7.17 ± 0.74% for the control cells after 24 h. The main detected metabolite in rat hepatocytes was the same as that detected in rat hepatic microsomes (the C29 monohydroxymethyl metabolite). Verapamil increased the quantity of MOX in the cells after 24, 48 and 72 h. Examination of the Area Under the concentration time Curve (AUC) of the main detected metabolite revealed a significant increase in the exposure of cells to MOX after verapamil treatment throughout the experiment. It is hypothesized that verapamil interfered with MOX as a substrate for Pgp during the initial incubation period. After this initial interaction, verapamil metabolites were able to interfere with Pgp. This experiment demonstrated the implication of Pgp in the transport of MOX and allowed prediction of the drug–drug interactions which might modify the bioavailability of endectocides.
Bibliography:ArticleID:JVP335
ark:/67375/WNG-7LQ3ZBXH-4
istex:0B5688C312FD26B857AF94EDD15E727C38654890
ISSN:0140-7783
1365-2885
DOI:10.1046/j.1365-2885.2001.00335.x