4.1 Article

Cerebral Cortical Microvascular Rarefaction in Metabolic Syndrome is Dependent on Insulin Resistance and Loss of Nitric Oxide Bioavailability

Journal

MICROCIRCULATION
Volume 22, Issue 6, Pages 435-445

Publisher

WILEY
DOI: 10.1111/micc.12209

Keywords

obesity; capillary density; rodent models of cardiovascular disease risk; perfusion

Funding

  1. Center for Cardiovascular and Respiratory Sciences
  2. Clinical and Translational Sciences Institute at the West Virginia University Health Sciences Center
  3. American Heart Association [IRG 14330015, PRE 16850005, EIA 0740129N]
  4. National Institutes of Health [U54GM104942, RR 2865AR, P20 RR 016477]
  5. National Institute of General Medical Sciences of the National Institutes of Health [U54GM104942]

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Objective: Chronic presentation of the MS is associated with an increased likelihood for stroke and poor stroke outcomes following occlusive cerebrovascular events. However, the physiological mechanisms contributing to compromised outcomes remain unclear, and the degree of cerebral cortical MVD may represent a central determinant of stroke outcomes. Methods: This study used the OZR model of MS and clinically relevant, chronic interventions to determine the impact on cerebral cortical microvascular rarefaction via immunohistochemistry with a parallel determination of cerebrovascular function to identify putative mechanistic contributors. Results: OZR exhibited a progressive rarefaction (to similar to 80% control MVD) of the cortical microvascular networks vs. lean Zucker rats. Chronic treatment with antihypertensive agents (captopril/hydralazine) had limited effectiveness in blunting rarefaction, although treatments improving glycemic control (metformin/rosiglitazone) were superior, maintaining similar to 94% control MVD. Chronic treatment with the antioxidant TEMPOL severely blunted rarefaction in OZR, although this ameliorative effect was prevented by concurrent NOS inhibition. Conclusions: Further analyses revealed that the maintenance of glycemic control and vascular NO bioavailability were stronger predictors of cerebral cortical MVD in OZR than was prevention of hypertension, and this may have implications for chronic treatment of CVD risk under stroke-prone conditions.

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