European Journal of Drug Metabolism and Pharmacokinetics 1999-01-01

Interaction of chlormezanone enantiomers with rat liver microsomes.

W Klinger, H Oelschläger, D Rothley, E Karge, A Seeling

Index: Eur. J. Drug Metab. Pharmacokinet. 24(1) , 63-8, (1999)

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Abstract

Both chlormezanone enantiomers, for the first time obtained by enantiospecific HPLC with a 100% yield, bind to oxidized cytochrome P-450 in rat liver microsomes with a binding curve according to type I, similar to hexobarbital but less pronounced. There are no differences between the binding curves of the two enantiomers. Ethylmorphine N-demethylation, ethoxycoumarin and ethoxyresorufin O-deethylation are inhibited by both chlormezanone enantiomers at 0.1-1 mM concentrations: no differences could be found. Luminol and lucigenin amplified chemiluminescence indicating the formation of reactive oxygen species was not influenced by either enantiomer in concentration ranges between millimolar and micromolar, whereas hydrogen peroxide formation was inhibited. NADPH/Fe stimulated lipid peroxidation was not influenced. Scavenger activity could not be demonstrated: the zymosan stimulated whole blood chemiluminescence was not influenced significantly.


Related Compounds

  • ethylmorphine

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