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Abstract

Bromobenzene metabolism in vivo and in vitro. The mechanism of 4-bromocatechol formation.

N E Miller, D Thomas and R E Billings
Drug Metabolism and Disposition May 1990, 18 (3) 304-308;
N E Miller
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D Thomas
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R E Billings
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Abstract

The metabolism of bromobenzene has been examined in isolated hepatocytes and liver microsomes from phenobarbital-induced rats and in phenobarbital-induced rats in vivo. The metabolite profile produced upon incubation of isolated rat hepatocytes with bromobenzene differed with the hepatocyte concentration. At a low hepatocyte concentration (0.5 x 10(6) cells/ml), 4-bromophenol was the major metabolite, while at higher hepatocyte concentrations (2.0 and 5.0 x 10(6) cells/ml) bromobenzene-3,4-dihydrodiol was the major metabolite. 4-Bromophenol was the primary metabolite in incubations with rat liver microsomes. In vivo, 3- and 4-bromophenol were more predominant, with very little dihydrodiol formed. 4-Bromocatechol, a potentially toxic metabolite of bromobenzene, was formed in vivo as well as in isolated hepatocytes and microsomes. However, the mechanism of catechol formation differed, as determined by the retention of a deuterium label at the para position of bromobenzene. In microsomes, 4-bromophenol was the predominant precursor metabolite of 4-bromocatechol. In isolated hepatocytes, although the relative contribution of 4-bromophenol as the bromocatechol precursor differed with hepatocyte concentration, bromobenzene-3,4-dihydrodiol was the predominant precursor at all concentrations. In vivo, as in isolated hepatocytes, 4-bromocatechol was formed primarily via bromobenzene-3,4-dihydrodiol.

 

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Drug Metabolism and Disposition
Vol. 18, Issue 3
1 May 1990
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Abstract

Bromobenzene metabolism in vivo and in vitro. The mechanism of 4-bromocatechol formation.

N E Miller, D Thomas and R E Billings
Drug Metabolism and Disposition May 1, 1990, 18 (3) 304-308;

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Abstract

Bromobenzene metabolism in vivo and in vitro. The mechanism of 4-bromocatechol formation.

N E Miller, D Thomas and R E Billings
Drug Metabolism and Disposition May 1, 1990, 18 (3) 304-308;
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