Literature DB >> 925482

Effects of ethinyl estradiol on hepatic microsomal proteins and the turnover of cytochrome P-450.

M Mackinnon, E Sutherland, F R Simon.   

Abstract

The effect of ethinyl estradiol, a steroid commonly used in birth control pills and possibly associated with impaired drug metabolism in humans, on the activity of and turnover of components of the hepatic microsomal mixed-function oxidase system was studied in male rats. After 5 days of ethinyl estradiol, 5 mg/kg/day, there was a significant decrease in the activity of ethylmorphine-N-demethylase and in cytochrome P-450, cytochrome b2, and NADPH cytochrome c reductase. Cytochrome P-450 apoproteins were identified within an SDS-polyacrylamide gel system, and the rate of turnover of cytochrome P-450 apoproteins was studied by double-isotope labeling techniques. After 5 days of ethinyl estradiol administration, the rate of degradation of cytochrome P-450 apoprotein was reduced (half-life of 50 hr compared to 24 hr in control), and their relative rate of synthesis was likewise reduced, indicating that a new steady state of protein turnover associated with reduced synthesis rate had been reached. This was confirmed by studies of the effect of ethinyl estradiol on the level of microsomal cytochrome P-450 over a 10-day period.

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Year:  1977        PMID: 925482

Source DB:  PubMed          Journal:  J Lab Clin Med        ISSN: 0022-2143


  17 in total

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4.  Effects of tobacco smoking and oral contraceptive use on theophylline disposition.

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5.  Experimental hepatobiliary injury. Comparison of in vivo drug elimination with in vitro drug-metabolizing enzyme capacity in the rat.

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6.  Impairment of caffeine clearance by chronic use of low-dose oestrogen-containing oral contraceptives.

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7.  Effect of chronic oral contraceptive steroids on theophylline disposition.

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9.  Antipyrine elimination in saliva after low-dose combined or progestogen-only oral contraceptive steroids.

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10.  Effects of oral contraceptive steroids (norethisterone/mestranol) on the activities of hepatic drug-metabolizing enzymes in iron-deficient anemic rats.

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