OBJECTIVE -This study compared the effects of nateglinide, glyburide, and placebo on postmeal glucose excursions and insulin secretion in previously diet-treated patients with type 2 diabetes.RESEARCH DESIGN AND METHODS -This randomized, double-blind, placebocontrolled multicenter study was conducted in 152 patients who received either nateglinide (120 mg before three meals daily, n ϭ 51), glyburide (5 mg q.d. titrated to 10 mg q.d. after 2 weeks, n ϭ 50), or placebo (n ϭ 51) for 8 weeks. Glucose, insulin, and C-peptide profiles during liquid meal challenges were measured at weeks 0 and 8. At weeks Ϫ1 and 7, 19-point daytime glucose and insulin profiles, comprising three solid meals, were measured.RESULTS -During the liquid-meal challenge, nateglinide reduced the incremental glucose area under the curve (AUC) more effectively than glyburide (⌬ ϭ Ϫ4.94 vs. Ϫ2.71 mmol ⅐ h/l, P Ͻ 0.05), whereas glyburide reduced fasting plasma glucose more effectively than nateglinide (⌬ ϭ Ϫ2.9 vs. Ϫ1.0 mmol/l, respectively, P Ͻ 0.001). In contrast, C-peptide induced by glyburide was greater than that induced by nateglinide (⌬ ϭ ϩ1.83 vs. ϩ0.95 nmol ⅐ h/l, P Ͻ 0.01), and only glyburide increased fasting insulin levels. During the solid meal challenges, nateglinide and glyburide elicited similar overall glucose control (⌬ 12-h incremental AUC ϭ Ϫ13.2 vs. Ϫ15.3 mmol ⅐ h/l), but the insulin AUC induced by nateglinide was significantly less than that induced by glyburide (⌬ 12-h AUC ϭ ϩ866 vs. ϩ1,702 pmol ⅐ h/l, P ϭ 0.01).CONCLUSIONS -This study demonstrated that nateglinide selectively enhanced early insulin release and provided better mealtime glucose control with less total insulin exposure than glyburide.
Diabetes Care 24:983-988, 2001
