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Journal of Pharmacology and Experimental Therapeutics

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Abstract

Hepatic metabolism of tolbutamide: characterization of the form of cytochrome P-450 involved in methyl hydroxylation and relationship to in vivo disposition.

R G Knodell, S D Hall, G R Wilkinson and F P Guengerich
Journal of Pharmacology and Experimental Therapeutics June 1987, 241 (3) 1112-1119;
R G Knodell
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S D Hall
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G R Wilkinson
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F P Guengerich
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Abstract

In vitro investigations suggest the same human liver cytochrome P-450 that catalyzes S-mephenytoin 4-hydroxylation, P-450MP, is responsible for methyl hydroxylation of the oral hypoglycemic agent tolbutamide. Tolbutamide hydroxylase activity copurified with P-450MP; electrophoretically homogenous P-450MP catalyzed both tolbutamide and S-mephenytoin hydroxylation. Each substrate competitively inhibited hydroxylation of the other, and anti-P-450MP inhibited tolbutamide hydroxylation in human liver microsomes. Significant correlation between tolbutamide and S-mephenytoin hydroxylase activities was seen in a set of human liver samples. These findings suggested that subjects with a genetically determined impairment in ability to hydroxylate mephenytoin might also have deficient tolbutamide metabolism. However, plasma tolbutamide concentration-time profiles and urinary excretion of metabolites formed via the hydroxylation pathway were similar in four phenotypically poor and six extensive metabolizers of mephenytoin. We suggest that alteration of a substrate binding site of P-450MP may reduce its ability to hydroxylate S-mephenytoin but not tolbutamide.

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Journal of Pharmacology and Experimental Therapeutics
Vol. 241, Issue 3
1 Jun 1987
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Abstract

Hepatic metabolism of tolbutamide: characterization of the form of cytochrome P-450 involved in methyl hydroxylation and relationship to in vivo disposition.

R G Knodell, S D Hall, G R Wilkinson and F P Guengerich
Journal of Pharmacology and Experimental Therapeutics June 1, 1987, 241 (3) 1112-1119;

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Abstract

Hepatic metabolism of tolbutamide: characterization of the form of cytochrome P-450 involved in methyl hydroxylation and relationship to in vivo disposition.

R G Knodell, S D Hall, G R Wilkinson and F P Guengerich
Journal of Pharmacology and Experimental Therapeutics June 1, 1987, 241 (3) 1112-1119;
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