Abstract
We are seeking to discover potent CNS-active sulfonylureas with structural features that allow for the formation of several types of prodrugs. We report herein the syntheses of compounds comprising an initial series of hydroxyl-substituted analogues of the potent ATP-sensitive potassium channel blockers glyburide (glibenclamide) and gliquidone. Somewhat unexpectedly, several of the compounds were found to be comparably potent to glyburide as inhibitors of specific [(3)H]glyburide binding in rat brain preparations.
Publication types
-
Research Support, Non-U.S. Gov't
MeSH terms
-
Animals
-
Brain / drug effects*
-
Brain / metabolism
-
Dose-Response Relationship, Drug
-
Glyburide / antagonists & inhibitors*
-
Glyburide / metabolism
-
Hydroxides / chemistry
-
Hydroxides / pharmacology*
-
Protein Binding / drug effects
-
Protein Binding / physiology
-
Rats
-
Sulfonylurea Compounds / chemistry
-
Sulfonylurea Compounds / pharmacology*
-
Synaptosomes / drug effects*
-
Synaptosomes / metabolism
-
Tritium / metabolism
Substances
-
Hydroxides
-
Sulfonylurea Compounds
-
Tritium
-
hydroxide ion
-
Glyburide