EFFECTS OF 3 RECOMBINANT HUMAN-LEUKOCYTE INTERFERONS ON DRUG-METABOLISM IN MICE
- 1 January 1982
- journal article
- research article
- Vol. 10 (6) , 579-585
Abstract
Three recombinant human leukocyte interferons (IFLrA, IFLrD and a hydrid IFLrA/D) that differ markedly in their antiviral activity in murine L cells were examined for their effects on hepatic microsomal drug metabolism in adult female CD-1 mice. When administered for 1 or 3 consecutive days, IFLrA/D, which exhibited the highest antiviral activity in murine L cells, caused a dose-dependent decrease in cytochrome P-450 content and in the rate of metabolism in vitro of benzo[a]pyrene, hexobarbital, 7-ethoxycoumarin, benzphetamine and zoxazolamine. The concentration of cytochrome b5 and the activity of NADPH-cytochrome c reductase were also depressed when IFLrA/D was administered for 3 days. Similar but smaller changes were observed following treatment of mice with IFLrD, which possessed .apprx. 1% of the antiviral activity of IFLrA/D in murine L cells. IFLrA, which was essentially devoid of antiviral activity in the mouse cell line failed to depress cytochrome P-450 levels and in vitro drug metabolism activity in a consistent or dose-dependent manner. Cytochrome P-450 content and the in vitro rate of metabolism of benzphetamine and zoxazolamine were maximally depressed 8-24 h after a single i.p. injection of 1.5 .mu.g interferon/mouse; at this time the interferons were no longer detectable in serum. Near-normal levels of cytochrome P-450 and in vitro drug metabolism activity were restored by 48 h after a single injection of interferon. Treatment of mice with 1.5 .mu.g of IFLrA/D once daily for 3 days prolonged hexobarbital sleeping time but not zoxazolamine paralysis time, whereas neither of these was influenced by treatment with IFLrA or D. An interferon-dependent process reduces the level of microsomal cytochrome P-450 in liver and potentiates the pharmacological actions of certain drugs in mice.This publication has 19 references indexed in Scilit:
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