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Stereoselective biotransformation of ketamine in equine liver and lung microsomes
Author(s) -
SCHMITZ A.,
PORTIER C. J.,
THORMANN W.,
THEURILLAT R.,
MEVISSEN M.
Publication year - 2008
Publication title -
journal of veterinary pharmacology and therapeutics
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 0.527
H-Index - 60
eISSN - 1365-2885
pISSN - 0140-7783
DOI - 10.1111/j.1365-2885.2008.00972.x
Subject(s) - biotransformation , microsome , ketamine , pharmacology , lung , stereoselectivity , chemistry , medicine , anesthesia , biochemistry , enzyme , catalysis
Stereoselectivity has to be considered for pharmacodynamic and pharmacokinetic features of ketamine. Stereoselective biotransformation of ketamine was investigated in equine microsomes in vitro . Concentration curves were constructed over time, and enzyme activity was determined for different substrate concentrations using equine liver and lung microsomes. The concentrations of R/S‐ketamine and R/S‐norketamine were determined by enantioselective capillary electrophoresis. A two‐phase model based on Hill kinetics was used to analyze the biotransformation of R/S‐ketamine into R/S‐norketamine and, in a second step, into R/S‐downstream metabolites. In liver and lung microsomes, levels of R‐ketamine exceeded those of S‐ketamine at all time points and S‐norketamine exceeded R‐norketamine at time points below the maximum concentration. In liver and lung microsomes, significant differences in the enzyme velocity ( V max ) were observed between S‐ and R‐norketamine formation and between V max of S‐norketamine formation when S‐ketamine was compared to S‐ketamine of the racemate. Our investigations in microsomal reactions in vitro suggest that stereoselective ketamine biotransformation in horses occurs in the liver and the lung with a slower elimination of S‐ketamine in the presence of R‐ketamine. Scaling of the in vitro parameters to liver and lung organ clearances provided an excellent fit with previously published in vivo data and confirmed a lung first‐pass effect.

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