Vascular Inflammation, Insulin Resistance, and Reduced Nitric Oxide Production Precede the Onset of Peripheral Insulin Resistance

doi:10.1161/ATVBAHA.108.169722

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Arteriosclerosis, Thrombosis, and Vascular Biology. 2008;28:1982-1988
Published online before print September 4, 2008, doi: 10.1161/ATVBAHA.108.169722

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(Arteriosclerosis, Thrombosis, and Vascular Biology. 2008;28:1982.)
© 2008 American Heart Association, Inc.

Integrative Physiology/Experimental Medicine

Vascular Inflammation, Insulin Resistance, and Reduced Nitric Oxide Production Precede the Onset of Peripheral Insulin Resistance

Francis Kim; Matilda Pham; Ezekiel Maloney; Norma O. Rizzo; Gregory J. Morton; Brent E. Wisse; Elizabeth A. Kirk; Alan Chait; Michael W. Schwartz

From the Department of Medicine (F.K., M.P., E.M., N.O.R., G.J.M., B.E.W., A.C., M.W.S.), Diabetes and Obesity Center of Excellence (F.K., G.J.M., B.E.W., A.C., M.W.S.), and the Department of Epidemiology and Nutritional Sciences Program (E.A.K.), University of Washington, Seattle.

Correspondence to Francis Kim, Department of Medicine, Box 359748, University of Washington, Seattle, WA 98104. E-mail fkim{at}u.washington.edu

Objectives— Obesity causes inflammation and insulin resistancein the vasculature as well as in tissues involved in glucosemetabolism such as liver, muscle, and adipose tissue. To investigatethe relative susceptibility of vascular tissue to these effects,we determined the time course over which inflammation and insulinresistance develops in various tissues of mice with diet-inducedobesity (DIO) and compared these tissue-based responses to changesin circulating inflammatory markers.

Methods and Results— Adult male C57BL/6 mice were fedeither a control low-fat diet (LF; 10% saturated fat) or a high-fatdiet (HF, 60% saturated fat) for durations ranging between 1to 14 weeks. Cellular inflammation and insulin resistance wereassessed by measuring phospho-I ${kappa}$ B ${alpha}$ and insulin-induced phosphorylationof Akt, respectively, in extracts of thoracic aorta, liver,skeletal muscle, and visceral fat. As expected, HF feeding inducedrapid increases of body weight, fat mass, and fasting insulinlevels compared to controls, each of which achieved statisticalsignificance within 4 weeks. Whereas plasma markers of inflammationbecame elevated relatively late in the course of DIO (eg, serumamyloid A [SAA], by Week 14), levels of phospho-I ${kappa}$ B ${alpha}$ in aorticlysates were elevated by 2-fold within the first week. The earlyonset of vascular inflammation was accompanied by biochemicalevidence of both endothelial dysfunction (reduced nitric oxideproduction; induction of intracellular adhesion molecule-1 andvascular cell adhesion molecule-1) and insulin resistance (impairedinsulin-induced phosphorylation of Akt and eNOS). Although inflammationand insulin resistance were also detected in skeletal muscleand liver of HF-fed animals, these responses were observed muchlater (between 4 and 8 weeks of HF feeding), and they were notdetected in visceral adipose tissue until 14 weeks.

Conclusions— During obesity induced by HF feeding, inflammationand insulin resistance develop in the vasculature well beforethese responses are detected in muscle, liver, or adipose tissue.This observation suggests that the vasculature is more susceptiblethan other tissues to the deleterious effects of nutrient overload.

Key Words: nitric oxide • vascular inflammation • eNOS • insulin resistance • obesity

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