Metabolism of vinylcyclooctane and partition ratio between epoxide formation and cytochrome P-450 destruction |
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Authors: | P.G. Gervasi L. Citti E. Testai G. Turchi |
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Affiliation: | Istifuto di Mutagenesi e Differemiamento CNR, Via Svezia 10, 56100-, Pisa, Italy |
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Abstract: | Vinylcyclooctane (VCO), which binds to the active site of cytochrome P-450 (P-450) giving a type I difference spectrum, has been found to form the corresponding epoxide as the main metabolite on treatment with liver microsomal monooxygenase obtained from phenobarbital-treated or untreated mice. During this metabolic process about 40% of the microsomal P-450 isozymes are destroyed, but the remainder still demethylates aminopyrine. Approx. 180 molecules of VCO are turned over and 132 of epoxyethylcyclooctane (EECO) are formed for each destructive event. |
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Keywords: | Vinylcyclooctane metabolism cytochrome P-450 inactivation difference spectra |
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