Horm Metab Res 1986; 18(9): 599-603
DOI: 10.1055/s-2007-1012384
Clinical

© Georg Thieme Verlag, Stuttgart · New York

Sulfonylurea Therapy Fails to Diminish Insulin Resistance in Type I-Diabetic Subjects

U. Keller, R. Müller, W. Berger
  • Department Innere Medizin, Kantonsspital Basel, Basel, Switzerland
Further Information

Publication History

1985

1985

Publication Date:
14 March 2008 (online)

Summary

To assess whether extrapancreatic effects of sulfonylureas in vivo are detectable in the absence of endogenous insulin secretion, insulin sensitivity was determined in six insulin-deficient type 1-diabetic subjects. Peripheral uptake and hepatic production of glucose and lipolysis were measured during hyperinsulinemia using the euglycemic clamp technique and 3-3H-glucose infusions twice, once during a period with glibornuride treatment (50 mg b.i.d.), and once without. Hepatic glucose production decreased in diabetic subjects during hyperinsulinemia (insulin infusion of 20 mU/m2 · min; plasma free insulin levels of 40±4 mU/l) from 2.9±0.6 mg/kg min to 0.2±0.1 mg/kg · min after 120 min, and plasma free fatty acid (FFA) concentrations decreased from 1.33±0.29 to 0.38±0.08 mmol/l. Hepatic production, peripheral uptake of glucose and plasma FFA concentrations before and during hyperinsulinemia were not influenced by pretreatment with glibornuride. Compared to 8 non-diabetic subjects, type 1-diabetics demonstrated a diminished effect of hyperinsulinemia on peripheral glucose clearance (2.4±0.04 vs 4.2±0.5 ml/kg·min, P < 0.01), whereas hepatic glucose production and plasma FFA levels were similarly suppressed by insulin. The data indicate that sulfonylurea treatment did not improve the diminished insulin sensitivity of peripheral glucose clearance in type 1-diabetic subjects; insulin action on hepatic glucose production and lipolysis was unimpaired in diabetics and remained uninfluenced by glibornuride. Thus, extrapancreatic effects of sulfonylureas in vivo are dependent on the presence of functioning β-cells.

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