Abstract

N-substituted cyclic imides of phthalimide, 2,3-dihydrohalazine-1,4 4-dione, and diphenimide were shown to reduce the serum uric acid levels in normal and hyperuric mice at 20 mg/kg/day I.P. for 14 days. The agents were potent inhibitors of commercial xanthine dehydrogenase and xanthine oxidase enzyme activities with IC 50 values from 10 −7 to 10 −8 M concentrations of drug.

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