Abstract
Ketamine is a widely used drug for its anesthetic and analgesic properties; it is also considered as a drug of abuse, as many cases of ketamine illegal consumption were reported. Ketamine isN-demethylated by liver microsomal cytochrome P450 into norketamine. The identification of the enzymes responsible for ketamine metabolism is of great importance in clinical practice. In the present study, we investigated the metabolism of ketamine in human liver microsomes at clinically relevant concentrations. Liver to plasma concentration ratio of ketamine was taken into consideration. Pooled human liver microsomes and human lymphoblast-expressed P450 isoforms were used. N-demethylation of ketamine was correlated with nifedipine oxidase activity (CYP3A4-specific marker reaction), and it was also correlated with S-mephenytoinN-demethylase activity (CYP2B6-specific marker reaction). Orphenadrine, a specific inhibitor to CYP2B6, and ketoconazole, a specific inhibitor to CYP3A4, inhibited theN-demethylation of ketamine in human liver microsomes. In human lymphoblast-expressed P450, the activities of CYP2B6 were higher than those of CYP3A4 and CYP2C9 at three concentrations of ketamine, 0.005, 0.05, and 0.5 mM. When these results were extrapolated using the average relative content of these P450 isoforms in human liver, CYP3A4 was the major enzyme involved in ketamineN-demethylation. The present study demonstrates that CYP3A4 is the principal enzyme responsible for ketamineN-demethylation in human liver microsomes and that CYP2B6 and CYP2C9 have a minor contribution to ketamineN-demethylation at therapeutic concentrations of the drug.
Footnotes
- Abbreviations used are::
- P450
- cytochrome P450
- NK
- norketamine
- Cli
- intrinsic clearance
- Received December 13, 2001.
- Accepted April 5, 2002.
- The American Society for Pharmacology and Experimental Therapeutics
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