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On the metabolic activation of benz[a]acridine and benz[c]acridine by rat liver and lung microsomes
Authors:Jürgen Jacob  Achim Schmoldt  Wolfgang Kohbrok  Gottfried Raab  Gernot Grimmer
Affiliation:1. Biochemisches Institut für Umweltcarcinogene, Ahrensburg, F.R.G.;2. Pharmakologisches Institut der Universität Hamburg F.R.G.
Abstract:The metabolism of benz[a]- and benz[c]acridine by liver and lung microsomes from untreated, phenobarbital (PB)-treated and benzo[k]fluoranthene (BkF)-treated rats has been studied by gas chromatography/mass spectrometry (GC/MS). Epoxidation and hydrolysis of the epoxides to dihydrodiols were found to be the predominant pathways for all substrates. N-Oxidation is likely to occur in the case of benz[c]acridine. However, no unequivocal evidence could be obtained for the formation of the ultimate carcinogens — the t-3,4-dihydrodiol-1,2-epoxides — in case of both benz[a]- and benz[c]acridine. K-Region oxidation was induced by phenobarbital, whereas the formation of non-K-region metabolites increased after BkF treatment in the case of benz[c]acridine.
Keywords:Address all correspondence to: Prof. Dr. Jürgen Jacob   Biochemisches Institut für Umweltcarcinogene   D-2070 Ahrensburg   Sieker Landstrasse 19   F.R.G.
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