AI Article Synopsis
- The study examined how sulfinpyrazone is processed in various animals after a specific dosage, focusing on its distribution and breakdown.
- In all tested species, the total levels of the drug and its metabolites in the blood matched the expected values, highlighting sulfinpyrazone and six of its metabolites as key components.
- Different species demonstrated distinct profiles in the presence of unchanged sulfinpyrazone and its metabolites, influencing the drug's effectiveness in inhibiting platelet aggregation based on plasma concentrations.
Article Abstract
1. The disposition and metabolism of sulfinpyrazone have been studied in rats, guinea-pigs, rabbits, dogs, rhesus monkeys and miniature swine after intravenous administration of 100 mg/kg of 14C-labelled drug. 2. In all species, the integrated plasma concentration (AUC, 0-24 h) of total radioactivity was almost completely covered by the sum of the AUC-values of unchanged sulfinpyrazone and six metabolites, i.e. the sulphide, the sulphone, p-hydroxy-sulfinpyrazone, the p-hydroxy-sulphide, the p-hydroxy-sulphone and 4-hydroxy-sulfinpyrazone. 3. Comparison of the plasma level profiles of unchanged sulfinpyrazone and the metabolites revealed pronounced differences between the species. Unchanged sulfinpyrazone was the most prominent compound in plasma of rats, dogs, monkeys and swine, whereas the sulphide metabolite predominated in guinea-pigs. In plasma of rabbits, these two compounds were found in similar amounts. 4. Species with predominant renal excretion of the 14C dose, i.e. rabbits, dogs and monkeys, eliminated sulfinpyrazone to a high extent unchanged. The renal excretion of the sulphide metabolite was low in all species. 5. Species differences in the biotransformation of sulfinpyrazone explain previously observed differences in inhibitory effect on platelet aggregation. This effect is intensive and long-lasting in species showing high plasma concentrations of the sulphide metabolite.
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| http://dx.doi.org/10.3109/00498258109045867 | DOI Listing |
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