Metabolism - Clinical and Experimental
Volume 44, Issue 12 , Pages 1519-1526, December 1995

Changes in insulin action and insulin secretion in the rat after dietary restriction early in life: Influence of dood restriction versus low-protein food restriction

  • Fraçoise Picarel-Blanchot

      Affiliations

    • Laboratoire Physiopathologie Nutrition, Centre National de la Recherche Scientifique (CNRS) Unite de Recherche Associee (URA) 307, Université D. Diderot, Paris, France
    • Instituto de Bioquimica, Centro Mixto Universidad Complutense y CSIC Facultad de Farmacia, Universidad Complutense, Madrid, Spain
  • ,
  • Carmen Alvarez

      Affiliations

    • Laboratoire Physiopathologie Nutrition, Centre National de la Recherche Scientifique (CNRS) Unite de Recherche Associee (URA) 307, Université D. Diderot, Paris, France
    • Instituto de Bioquimica, Centro Mixto Universidad Complutense y CSIC Facultad de Farmacia, Universidad Complutense, Madrid, Spain
  • ,
  • Danielle Bailbe

      Affiliations

    • Laboratoire Physiopathologie Nutrition, Centre National de la Recherche Scientifique (CNRS) Unite de Recherche Associee (URA) 307, Université D. Diderot, Paris, France
    • Instituto de Bioquimica, Centro Mixto Universidad Complutense y CSIC Facultad de Farmacia, Universidad Complutense, Madrid, Spain
  • ,
  • Ana-Maria Pascual-Leone

      Affiliations

    • Laboratoire Physiopathologie Nutrition, Centre National de la Recherche Scientifique (CNRS) Unite de Recherche Associee (URA) 307, Université D. Diderot, Paris, France
    • Instituto de Bioquimica, Centro Mixto Universidad Complutense y CSIC Facultad de Farmacia, Universidad Complutense, Madrid, Spain
  • ,
  • Bernard Portha

      Affiliations

    • Corresponding Author InformationAddress reprint requests to Bernard Portha, PhD, Lab. Physiopathology of Nutrition, CNRS URA 307, Université D. Diderot/Paris 7, 2 place Jussieu, Tour 33, 75251 Paris Cedex 05, France
    • Laboratoire Physiopathologie Nutrition, Centre National de la Recherche Scientifique (CNRS) Unite de Recherche Associee (URA) 307, Université D. Diderot, Paris, France
    • Instituto de Bioquimica, Centro Mixto Universidad Complutense y CSIC Facultad de Farmacia, Universidad Complutense, Madrid, Spain

Received 4 June 1994; accepted 18 April 1995.

Abstract 

The effect of a limited period of undernutrition in young rats on insulin secretion and insulin action during adulthood has been studied. Four-week-old female rats were either food-restricted (35% restriction, 15% protein diet) or protein-calorie-restricted (35% restriction, 5% protein diet) for 4 weeks. Food-restricted rats gained weight at a lower rate than control rats. In the protein-calorie-restricted group, the alteration of weight gain was more severe. Basal plasma insulin was reduced only in protein-calorie-restricted rats. Glucose-stimulated insulin secretion (ΔI) obtained in vivo after an intravenous glucose load was only moderately decreased in food-restricted group, whereas it was severely blunted in the protein-calorie-restricted group. In this last group, impairment of the insulin secretory response to glucose was related to an intrinsic impairment of β-cell secretory capacity, since the insulin secretory response to glucose or arginine was decreased when tested in vitro (perfused pancreas). In food-restricted rats, basal plasma glucose level was kept normal, while a mild deterioration of glucose tolerance was detectable. This was related, of course, to the decrease of ΔI as identified in vivo. However, data obtained under basal or euglycemic-hyperinsulinemic conditions provided direct evidence that insulin-mediated total glucose uptake (weight-related expression) was paradoxically enhanced. A similar conclusion was reached in protein-calorie-restricted rats; the increase of overall insulin-mediated glucose uptake was even more important. Such an adaptation, which was operating in both types of restriction, may help limit the deterioration of glucose tolerance in the face of impaired insulin release. In the basal postabsorptive state, the higher glucose utilization rate in both models originated from increased hepatic glucose production rates. During hyperinsulinemia, endogenous glucose production in food-restricted rats was normally blunted, but not in protein-calorie-restricted rats, thus indicating resistance of the hepatic glucose production pathway to insulin action in this group.

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 Supported in part by the France/Spain Programme for Science (Actions Intégrées 149 and 216 and Cooperation Franco-Espagnole CNRS/CSIC project 1986). C.A. was the recipient of a fellowship from Université D. Diderot / Paris 7 (Maitre de Conference invite, emploi no. 234MA0202).

PII: 0026-0495(95)90068-3

Metabolism - Clinical and Experimental
Volume 44, Issue 12 , Pages 1519-1526, December 1995