Diazepam metabolism in human foetal and adult liver |
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Authors: | E. Ackermann K. Richter |
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Affiliation: | (1) Institute for Clinical Pharmacology Carl Gustav Carus, Dresden, German Democratic Republic;(2) Zentralinstitut für Krebsforschung, Akademie der Wissenschaften der DDR, Lindenberger Weg 80, DDR-1115 Berlin, German Democratic Republic |
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Abstract: | Summary Diazepam was metabolized by human foetal liver microsomes to N-desmethyldiazepam and N-methyloxazepam as early as the 13th week of gestation. The metabolic activity was lower than that of microsomes from adult human liver. Diazepam was shown mainly to be hydroxylated to N-methyloxazepam at substrate concentrations higher than 0.1 mM. Diazepam levels above 1.0 mM were inhibitory to the overall metabolic reaction. SKF 525-A inhibited diazepam metabolism by foetal liver microsomes at a concentration of 0.1 mM. The addition of diazepam to foetal and adult human liver microsomes resulted in a type II spectral change. Its inhibition by carbon monoxide indicated that biotransformation of diazepam was performed by the cytochrome P-450-linked mono-oxygenase system. |
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Keywords: | Diazepam liver microsomes human foetus and adult metabolism spectral change SKF 525-A CO cytochrome P-450 |
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