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Publication : Endothelial Estrogen Receptor-α Does Not Protect Against Vascular Stiffness Induced by Western Diet in Female Mice.

First Author  Manrique C Year  2016
Journal  Endocrinology Volume  157
Issue  4 Pages  1590-600
PubMed ID  26872089 Mgi Jnum  J:234303
Mgi Id  MGI:5789693 Doi  10.1210/en.2015-1681
Citation  Manrique C, et al. (2016) Endothelial Estrogen Receptor-alpha Does Not Protect Against Vascular Stiffness Induced by Western Diet in Female Mice. Endocrinology 157(4):1590-600
abstractText  Consumption of a diet high in fat and refined carbohydrates (Western diet [WD]) is associated with obesity and insulin resistance, both major risk factors for cardiovascular disease (CVD). In women, obesity and insulin resistance abrogate the protection against CVD likely afforded by estrogen signaling through estrogen receptor (ER)alpha. Indeed, WD in females results in increased vascular stiffness, which is independently associated with CVD. We tested the hypothesis that loss of ERalpha signaling in the endothelium exacerbates WD-induced vascular stiffening in female mice. We used a novel model of endothelial cell (EC)-specific ERalpha knockout (EC-ERalphaKO), obtained after sequential crossing of the ERalpha double floxed mice and VE-Cadherin Cre-recombinase mice. Ten-week-old females, EC-ERalphaKO and aged-matched genopairs were fed either a regular chow diet (control diet) or WD for 8 weeks. Vascular stiffness was measured in vivo by pulse wave velocity and ex vivo in aortic explants by atomic force microscopy. In addition, vascular reactivity was assessed in isolated aortic rings. Initial characterization of the model fed a control diet did not reveal changes in whole-body insulin sensitivity, aortic vasoreactivity, or vascular stiffness in the EC-ERalphaKO mice. Interestingly, ablation of ERalpha in ECs reduced WD-induced vascular stiffness and improved endothelial-dependent dilation. In the setting of a WD, endothelial ERalpha signaling contributes to vascular stiffening in females. The precise mechanisms underlying the detrimental effects of endothelial ERalpha in the setting of a WD remain to be elucidated.
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