Article

Effect of Endothelium-Specific Insulin Resistance on Endothelial Function In Vivo

Edward DuncanCardiovascular Division, Department of Cardiology, King's College London, U.KPaul A. CrosseyCardiovascular Division, Department of Cardiology, King's College London, U.KSimon WalkerCardiovascular Division, Department of Cardiology, King's College London, U.KNarayana AnilkumarCardiovascular Division, Department of Cardiology, King's College London, U.KLucilla PostonMaternal and Fetal Research Unit, Division of Reproduction and Endocrinology, King's College London, London, U.KGillian DouglasMaternal and Fetal Research Unit, Division of Reproduction and Endocrinology, King's College London, London, U.KVivienne EzzatCardiovascular Division, Department of Cardiology, King's College London, U.KStephen B. WheatcroftCardiovascular Division, Department of Cardiology, King's College London, U.KAjay M. ShahCardiovascular Division, Department of Cardiology, King's College London, U.KMark KearneyCardiovascular Division, Department of Cardiology, King's College London, U.K

2008en

ABI

Abstract

OBJECTIVE: Insulin resistance is an independent risk factor for the development of cardiovascular atherosclerosis. A key step in the development of atherosclerosis is endothelial dysfunction, manifest by a reduction in bioactivity of nitric oxide (NO). Insulin resistance is associated with endothelial dysfunction; however, the mechanistic relationship between these abnormalities and the role of impaired endothelial insulin signaling versus global insulin resistance remains unclear. RESEARCH DESIGN AND METHODS: To examine the effects of insulin resistance specific to the endothelium, we generated a transgenic mouse with endothelium-targeted overexpression of a dominant-negative mutant human insulin receptor (ESMIRO). This receptor has a mutation (Ala-Thr(1134)) in its tyrosine kinase domain that disrupts insulin signaling. Humans with the Thr(1134) mutation are insulin resistant. We performed metabolic and vascular characterization of this model. RESULTS: ESMIRO mice had preserved glucose homeostasis and were normotensive. They had significant endothelial dysfunction as evidenced by blunted aortic vasorelaxant responses to acetylcholine (ACh) and calcium ionophore. Furthermore, the vascular action of insulin was lost in ESMIRO mice, and insulin-induced endothelial NO synthase (eNOS) phosphorylation was blunted. Despite this phenotype, ESMIRO mice demonstrate similar levels of eNOS mRNA and protein expression to wild type. ACh-induced relaxation was normalized by the superoxide dismutase mimetic, Mn(III)tetrakis(1-methyl-4-pyridyl) porphyrin pentachloride. Endothelial cells of ESMIRO mice showed increased superoxide generation and increased mRNA expression of the NADPH oxidase isoforms Nox2 and Nox4. CONCLUSIONS: Selective endothelial insulin resistance is sufficient to induce a reduction in NO bioavailability and endothelial dysfunction that is secondary to increased generation of reactive oxygen species. This arises independent of a significant metabolic phenotype.

Identifiers

DOI: 10.2337/db07-1111

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