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Christian Rask-Madsen
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Title
Assistant Professor
Expertise
Cardiovascular
Institution
Joslin Diabetes Center - Boston
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Insulin action on endothelium in angiogenesis
Patients with obesity and type 2 diabetes have increased risk for heart failure and limb amputation, in part because of impaired neovascular response in hypoxic tissue. Insulin action directly on vascular endothelium can activate proangiogenic mechanisms such as generation of nitric oxide (NO). Therefore, insulin resistance in endothelial cells could help explain compromised neovascularization in ischemic tissues in conditions with insulin resistance. Based on strong preliminary data, we hypothesize that insulin action on endothelial cells, through inhibition of the transcription factor FoxO, can regulate angiogenic or angiostatic genes and thereby promote angiogenesis in muscle. In Aim 1, we will determine the contribution to angiogenesis of insulin receptor signaling in endothelial cells. Blood flow, collateral formation, and angiogenesis will be quantitated in the ischemic hindlimb after femoral artery ligation and compared with these parameters in the contralateral leg, using mice with knockout of the insulin receptor restricted to endothelial cells or their littermate controls. In Aim 2, we will determine the relative contribution of FoxO1 or FoxO3 to insulin signaling and cell function in endothelial cell culture by adenovirus-mediated expression of FoxO constructs. We will also screen for insulin-stimulated regulation of 23 genes previously documented as being regulated by FoxO and determine which of these genes mediate proangiogenic cell function by shRNA-mediated knockdown of candidate genes using lentivirus as vectors. Relevance. This work will provide an animal model of impaired angiogenesis in conditions with insulin resistance and identify insulin-regulated genes in endothelial cells which modifies angiogenesis. Ultimately, results from this research may guide development of insulin analogs and insulin sensitizers and identify novel targets for improving heart and limb function in complications of obesity and type 2 diabetes.
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Insulin action on endothelium in angiogenesis (Rask-Madsen, Christian)
11/26/2013
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The DiaComp Steering Committee is the governing body of the consortium. The principle function of this committee is to guide the scientific direction of the consortium. This is accomplished by creating various subcommittees necessary to advance the scientific goals and providing guidance to the broader complications research community. Policies for the consortium are developed through consultation with the
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Cardiovascular
The DiaComp Cardiovascular Committee has the principal function of furthering the mission of the consortium with regard to diabetic cardiomyopathy and macrovascular disease.
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Please acknowledge all posters, manuscripts or scientific materials that were generated in part or whole using funds from the Diabetic Complications Consortium(DiaComp) using the following text:
Financial support for this work provided by the NIDDK Diabetic Complications Consortium (RRID:SCR_001415, www.diacomp.org), grants DK076169 and DK115255
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