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Molecular Pharmacology, Vol 20, 442-450, Copyright © 1981 by the American Society for Pharmacology and Experimental Therapeutics
1 McArdle Laboratory for Cancer Research, University of Wisconsin, Madison, Wisconsin 53706
1,4-Bis[2-(3,5-dichloropyridyloxy)]-benzene (TCPOBOP), previously shown to be an extremely potent inducer of the phenobarbital pleiotropic response in mice, was surprisingly
ineffective in the rat. Hepatic aminopyrine N-demethylase, benzphetamine N-demethylase, NADPH-cytochrome c reductase, microsomal epoxide hydrolase and 
aldehyde
dehydrogenase activities, cytochrome P-450, and liver weight were all increased in the rat
by sodium phenobarbital, but not by TCPOBOP at a dose of 10 mg/kg (equivalent to 50
times the mouse ED50). At higher doses, TCPOBOP did produce an increase in hepatic
benzphetamine N-demethylase activity, but this response plateaued at about 40% of the
maximal response produced by phenobarbital. TCPOBOP appears to have diminished
potency and intrinsic activity in the rat, but it does not antagonize the effect of
phenobarbital (i.e., act as a partial agonist). In four strains of mice and Syrian golden
hamsters, TCPOBOP (3 mg/kg) was a potent inducer of hepatic aminopyrine N-demethylase activity, but four strains of rats and guinea pigs failed to respond. This greatly
diminished potency of TCPOBOP in the rat (ED50 1.2 x 10-4 moles/kg) compared with
the mouse (ED50 = 4.9 x 10-7 moles/kg) is not attributable to (a) a rapid metabolism or
excretion, because in both species [3H] TCPOBOP has a long half-life and is stored
primarily as the parent compound; or (b) a toxic effect preventing the hepatic induction
response. The species difference in sensitivity to TCPOBOP appears to be due to some
evolutionary change affecting the mechanism of induction by TCPOBOP but not by
phenobarbital.
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