Comparison of Pharmacokinetics, Metabolic Effects and Mechanisms of Action of Glyburide and Glipizide During Long-Term Treatment

Author:

Groop Leif1,Groop Per-Henrik1,Stenman Svante1,Saloranta Carola1,Tötterman Karl-Johan1,Fyhrquist Frej1,Melander Arne2

Affiliation:

1. Fourth Department of Medicine, Helsinki University Hospital Helsinki Finland

2. Division of Clinical Pharmacology, Department of Research in Primary Health Care, Lund University Health Science Center Dalby, Sweden

Abstract

Fourteen non-insulin-dependent diabetic (NIDDM) patients continued their previous medication (7 on glyburide, 7 on glipizide) for 6 mo, after which they switched to the alternate treatment for another 6 mo. The treatment periods were followed by 1 mo of placebo. The sulfonylurea dose was increased to achieve fasting plasma glucose levels <9 mM or to a total maximum daily dose of 25 mg. The mean final doses of glyburide (14.7 ± 2.4 mg/day) and glipizide (15.2 ± 2.2 mg/day) were similar. Postprandial (postdose) glipizide levels were higher than those of glyburide, whereas fasting (predose) glyburide concentrations were higher than those of glipizide. Both treatments improved glucose controlby 25% compared with placebo. Glipizide therapy evoked higher postprandial insulin concentrations than did glyburide, whereas basal insulin concentrations were higher during glyburide. Insulin sensitivity, assessed by an insulin tolerance test, was more improved with glyburide than with glipizide. In conclusion, overall glucose control is similarly improved by glyburide and glipizide. However, glipizide amplifies the plasma insulin response to meals more than glyburide, whereas glyburide enhances basal insulin secretion more than glipizide. Both pharmacokinetic and pharmacodynamic factors may contribute to these differences.

Publisher

American Diabetes Association

Subject

Advanced and Specialized Nursing,Endocrinology, Diabetes and Metabolism,Internal Medicine

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