Obesity and insulin resistance in humans: a dose-response study

Insulin-mediated glucose metabolism (euglycemic insulin clamp at plasma insulin concentration of 100 microU/mL) and glucose-stimulated insulin secretion (hyperglycemic clamp) were examined in 42 obese subjects (ideal body weight [IBW], 158 +/- 4%) with normal glucose tolerance and in 36 normal weigh...

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Published inMetabolism, clinical and experimental Vol. 39; no. 5; pp. 452 - 459
Main Authors Bonadonna, R.C, Groop, L, Kraemer, N, Ferrannini, E, Del Prato, S, DeFronzo, R.A
Format Journal Article
LanguageEnglish
Published United States 01.05.1990
Subjects
adipose tissue
Adult
Blood Glucose - metabolism
blood plasma
Dose-Response Relationship, Drug
Female
glucose
Glucose - pharmacokinetics
Glucose Clamp Technique
Humans
insulin
Insulin - blood
Insulin - metabolism
Insulin Resistance
Insulin Secretion
Liver - metabolism
Male
metabolism
obesity
Obesity - blood
resistance
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Summary:Insulin-mediated glucose metabolism (euglycemic insulin clamp at plasma insulin concentration of 100 microU/mL) and glucose-stimulated insulin secretion (hyperglycemic clamp) were examined in 42 obese subjects (ideal body weight [IBW], 158 +/- 4%) with normal glucose tolerance and in 36 normal weight (IBW, 102% +/- 1%) age-matched controls. In 10 obese and eight control subjects, insulin was infused at six rates to increase plasma insulin concentration by approximately 10, 20, 40, 80, 2,000, and 20,000 microU/mL. Throughout the physiologic range of plasma insulin concentrations, both the increase in total body glucose uptake and the suppression of hepatic glucose production (HGP) were significantly impaired in the obese group (P less than .001 to .01). At the two highest plasma insulin concentrations, inhibition of HGP and the stimulation of glucose disposal were similar in both the obese and control groups. Insulin secretion during the hyperglycemic (+/- 125 mg/dL) clamp was twofold greater in obese subjects than in controls (P less than .01) and was inversely related to the rate of glucose uptake during the insulin clamp (r = -.438, P less than .05), but was still unable to normalize glucose disposal (P less than .05). In conclusion, our results indicate that insulin resistance is a common accompaniment of obesity and can be overcome at supraphysiological insulin concentrations. Both in the basal state and following a hyperglycemic stimulus obese people display hyperinsulinemia, which correlates with the degree of insulin resistance. However, endogenous hyperinsulinemia fails to fully compensate for the insulin resistance.
ISSN:0026-0495
1532-8600
DOI:10.1016/0026-0495(90)90002-T