The effect of ethanol on drug oxidations <i>in vitro</i> and the significance of ethanol–cytochrome <i>P</i>-450 interaction

Cinti, Dominick L.; Grundin, Robert; Orrenius, Sten

doi:10.1042/bj1340367

Cited by 66 publications

(20 citation statements)

References 28 publications

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“…In liver slices, Cinti et al (1973) observed at low ethanol concentrations an enhanced rate of drug oxidation, probably as a result of increased NADH con centration. The same authors report an inhibition of microsomal drug metab olism in microsomal suspensions at high ethanol concentrations and attributed this to interference of ethanol with binding of drug substrates to cytochrome P-450.…”

Section: Discussionmentioning

confidence: 99%

Interaction between Antipyrine and the Microsomal Ethanol Oxidation in Rat Liver

Andreasen¹,

Bremmelgaard²,

Larsen³

1974

Pharmacology

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Section: Discussionmentioning

confidence: 99%

Interaction between Antipyrine and the Microsomal Ethanol Oxidation in Rat Liver

Andreasen¹,

Bremmelgaard²,

Larsen³

1974

Pharmacology

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“…This could be explained by the fact that in this experiment larger quantities of ethanol were administered, and, according to Cinti el al. [12], low doses of ethanol stimulate, whereas higher doses inhibit microsomal enzymes. Any dose level above 5 % v/v in water is regarded as producing liver damage [7] and this could explain the decrease in aryl hydrocarbon hydroxylase observed here.…”

Section: Discussionmentioning

confidence: 99%

“…Following intraperitoneal injection the microsomal protein and, correspondingly, the levels of the various components of the MEOS arc reduced. After oral in take the protein, initially lowered, recovers -presumably by the induction of the MEOS which has been reported for lower ethanol concentrations [12). The level to which the MEOS can be induced will be greatly influenced by the diet, especially the amount of lipid present [7j.…”

Section: Discussionmentioning

confidence: 99%

The Effect of Chronic Alcohol Intake Upon the Hepatic Microsomal Carcinogen-activation System

Capel¹,

Jenner²,

Pinnock³

et al. 1978

Oncology

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Ethanol was administered to mice either by repeated intraperitoneal injection, or orally in the drinking water over an extended period of time. Following intraperitoneal ethanol pre-treatment further groups of mice received an injection of benzo(a)pyrene. Alcohol intake decreased the level of microsomal aryl hydrocarbon hydroxylase which corresponded to the observed decrease in DNA binding of benzo(a)pyrene. In contrast, the number of tumors which developed in the alcohol pre-treated mice exceeded those of the control animals.

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“…The levels of ethanol required to inhibit the metabolism of most drugs by the hepatic microsomal fraction, around 100 mM (Rubin et al, 1970;Cinti, Grundin & Orrenius, 1973), are in general higher than those encountered except under cases of severe intoxication. It was of interest therefore to examine in vivo drug clearances several hours after a single dose of ethanol, when the ethanol had been completely removed from the blood.…”

mentioning

confidence: 93%

PROCEEDINGS OF THE British Pharmacological Society

1977

British J Pharmacology

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The effect of ethanol on drug oxidations in vitro and the significance of ethanol–cytochrome P-450 interaction

Cited by 66 publications

References 28 publications

Interaction between Antipyrine and the Microsomal Ethanol Oxidation in Rat Liver

Interaction between Antipyrine and the Microsomal Ethanol Oxidation in Rat Liver

The Effect of Chronic Alcohol Intake Upon the Hepatic Microsomal Carcinogen-activation System

PROCEEDINGS OF THE British Pharmacological Society

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