Initial steps of insulin signaling and glucose transport are defective in the type 2 diabetic rat heart

doi:10.1016/j.cardiores.2003.11.021

Cardiovascular Research 2004 61(2):288-296; doi:10.1016/j.cardiores.2003.11.021
© 2004 by European Society of Cardiology

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Initial steps of insulin signaling and glucose transport are defective in the type 2 diabetic rat heart

Martine Desrois^a^,*, Robert J Sidell^a, Dominique Gauguier^b, Linda M King^a, George K Radda^a and Kieran Clarke^a

^aUniversity Laboratory of Physiology, University of Oxford, Oxford, England, UK
^bThe Wellcome Trust Centre for Human Genetics, University of Oxford, Oxford, England, UK

^* Corresponding author. Centre de Résonance Magnétique Biologique et Médicale (CRMBM) UMR CNRS 6612, Faculté de Médecine, 27 Bd Jean Moulin, 13005 Marseille, France. Tel.: +33-4-91256529; fax: +33-4-91256539. martine.desrois{at}medecine.univ-mrs.fr

Objective: Whole body insulin resistance and diabetes are riskfactors for cardiovascular diseases, yet little is known aboutinsulin resistance in the diabetic heart. The aim of this workwas to define the insulin response in hearts of the Goto–Kakizaki(GK) rat, a polygenic model of spontaneous type 2 diabetes.Methods: We measured D[2-³H]glucose uptake before and afterinsulin stimulation, plus initial steps of the insulin signalingpathway after insulin infusion via the caudal vena cava in heartsfrom the male Wistar and spontaneously diabetic GK rats. Results:Despite normal basal D[2-³H]glucose uptake, insulin-stimulatedglucose uptake was 50% (p<0.03) lower in GK rat hearts comparedwith their Wistar controls. Total GLUT4 protein was depletedby 28% (p<0.01) in GK rat hearts. We found 31% (p<0.0001)and 38% (p<0.001) decreased protein levels of insulin receptorβ (IRβ)-subunit and insulin receptor substrate-1 (IRS-1),respectively, in GK rat hearts with 37% (p<0.02) and 45%(p<0.01) lower insulin-stimulated tyrosine phosphorylationof these proteins. Owing to the decreased IRS-1 protein levels,GK rat hearts had a 41% (p<0.0001) decrease in insulin-stimulatedIRS-1 protein association with the p85 subunit of phosphatidylinositol3-kinase, despite normal phosphatidylinositol 3-kinase proteinexpression. Insulin-stimulated serine phosphorylation of proteinkinase B was the same in all hearts, as was protein kinase Bexpression. Conclusion: We conclude that decreased insulin receptorβ, IRS-1 and GLUT4 proteins are associated with insulinresistance in type 2 diabetic rat hearts.

KEYWORDS Diabetes; Signal transduction; Protein phosphorylation; Receptors; Membrane transport

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