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Abstract

Mechanism of metabolic cleavage of a furan ring.

T Kobayashi, J Sugihara and S Harigaya
Drug Metabolism and Disposition November 1987, 15 (6) 877-881;
T Kobayashi
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J Sugihara
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S Harigaya
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Abstract

We studied the mechanism of metabolic cleavage of a furan ring, using a new hypolipidemic agent, ethyl 2-(4-chlorophenyl)-5-(2-furyl)oxazole-4-acetate (TA-1801), as a model compound. A TA-1801 analogue labeled with deuterium at the 5-position of its furan ring was administered orally to rats. The analysis of urinary metabolites by GC/MS revealed that the deuterium of the furan was retained in the ring-opened metabolite (M3). Metabolic cleavage of furan has been generally considered to proceed by hydroxylation of the 5-position followed by tautomerism and hydrolysis of the resulting 5-hydroxyfuran derivative. However, if the cleavage proceeded by this pathway, the deuterium of the 5-position would be eliminated during hydroxylation. Therefore, we propose that the ring was cleaved directly to form an unsaturated aldehyde, considering the mechanism of oxidation by cytochrome P-450. Although this "intermediate" was not detected in the biological specimens, a synthetic unsaturated aldehyde was transformed to the actual urinary metabolites M2 and M3 (major ring-opened metabolites) in the isolated rat liver.

 

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Drug Metabolism and Disposition
Vol. 15, Issue 6
1 Nov 1987
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Abstract

Mechanism of metabolic cleavage of a furan ring.

T Kobayashi, J Sugihara and S Harigaya
Drug Metabolism and Disposition November 1, 1987, 15 (6) 877-881;

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Abstract

Mechanism of metabolic cleavage of a furan ring.

T Kobayashi, J Sugihara and S Harigaya
Drug Metabolism and Disposition November 1, 1987, 15 (6) 877-881;
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