George J. Traiger scite author profile

A pharmacokinetic model is presented to describe the biotransformation of 2-butanol (2-OL) and its metabolites (2-butanone, 3-hydroxy-2-butanone, and 2, 3-butanediol) using in vivo experimental blood concentration. A flow limited model is developed to simulate 2-OL, 2-butanone (2-ONE), 3-hydroxy-2-butanone (3H-2B), and 2,3-butanediol (2,3-RD) blood concentrations in rats after oral administration of 2-OL. Assuming the only important site of 2-OL biotransformation is the liver, the tissues included are the liver and a volume of distribution, essentially body water in the case of 2-OL and its metabolites. A distribution coefficient is found to be necessary to describe the low concentration of 3H-2B in blood after administration of 2-OL. The need for this coefficient may be due to partitioning, binding, or altered transport rates from the liver. Inhibition of 2-ONE metabolism to 3H-2B by 2-OL has been included to explain a time delay in the appearance of 3H-2B after administration of 2-OL. Subsequent experimental verification confirms the mixed function oxidase inhibitory properties of 2-OL. The model is able to simulate blood concentrations and elimination of all four compounds after the oral administration of 2-OL. Additionally, the model also simulates the results obtained after i.v. administration of 3H-3B and 2,3-BD.

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Toxicity-distribution relationships among 3-alkylfurans in mouse liver and kidney

Wiley

Traiger

Baraban

et al. 1984

Toxicology and Applied Pharmacology

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Relative hepatotoxicity of substituted thiobenzamides and thiobenzamide-S-oxides in the rat

Hanzlik

Cashman

Traiger

1980

Toxicology and Applied Pharmacology

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Differences in the potentiation of carbon tetrachloride in rats by ethanol and isopropanol pretreatment

Traiger

Plaa

1971

Toxicology and Applied Pharmacology

143

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George J. Traiger

Preliminary Safety Evaluation of Parenterally Administered Sulfoalkyl Ether β-Cyclodextrin Derivatives

Pharmacokinetics of 2-butanol and its metabolites in the rat

Toxicity-distribution relationships among 3-alkylfurans in mouse liver and kidney

Relative hepatotoxicity of substituted thiobenzamides and thiobenzamide-S-oxides in the rat

Differences in the potentiation of carbon tetrachloride in rats by ethanol and isopropanol pretreatment

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