Glp-1 And Insulin Recruit Muscle Microvasculature And Dilate Conduit Artery Individually But Not Additively In Healthy Humans

JOURNAL OF THE ENDOCRINE SOCIETY(2018)

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Abstract
Context: Glucagon-like peptide-1 (GLP-1) and insulin increase muscle microvascular perfusion, thereby increasing tissue endothelial surface area and nutrient delivery.Objective: To examine whether GLP-1 and insulin act additively on skeletal and cardiac microvasculature and conduit artery.Design: Healthy adults underwent three study protocols in random order.Setting: Clinical Research Unit at the University of Virginia.Methods: Overnight-fasted participants received an intravenous infusion of GLP-1 (1.2 pmol/kg/min) or normal saline for 150 minutes with or without a 2-hour euglycemic insulin clamp (1mU/kg/min) superimposed from 30 minutes onward. Skeletal and cardiac muscle microvascular blood volume (MBV), flow velocity, and flow; brachial artery diameter, flow velocity, and blood flow; and pulse wave velocity (PWV) were measured.Results: GLP-1 significantly increased skeletal and cardiac muscle MBV and microvascular blood flow (MBF) after 30 minutes; these remained elevated at 150 minutes. Insulin also increased skeletal and cardiac muscle MBV and MBF. Addition of insulin to GLP-1 did not further increase skeletal and cardiac muscle MBV and MBF. GLP-1 and insulin increased brachial artery diameter and blood flow, but this effect was not additive. Neither GLP-1, insulin, nor GLP-1 and insulin altered PWV. Combined GLP-1 and insulin infusion did not result in higher whole-body glucose disposal.Conclusion: GLP-1 and insulin at physiological concentrations acutely increase skeletal and cardiac muscle microvascular perfusion and dilate conduit artery in healthy adults; these effects are not additive. Thus, GLP-1 and insulin may regulate skeletal and cardiac muscle endothelial surface area and nutrient delivery under physiological conditions. Copyright (c) 2018 Endocrine Society
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Key words
conduit artery, heart perfusion, incretin, insulin, microvascular recruitment, muscle perfusion
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