Preclinical Modeling of Metabolic Syndrome to Study the Pleiotropic Effects of Novel Antidiabetic Therapy Independent of Obesity

Author:

Mochel Jonathan P.1,Ward Jessica L.2,Blondel Thomas3,Kundu Debosmita2,Merodio Maria M.2,Zemirline Claudine3,Guillot Emilie3,Giebelhaus Ryland T.4,Mata Paulina4,Iennarella-Servantez Chelsea A.2,Blong April2,Nam Seo Lin4,Harynuk James J.4,Suchodolski Jan5,Tvarijonaviciute Asta6,Cerón José Joaquín6,Bourgois-Mochel Agnes1,Zannad Faiez7,Sattar Naveed8,Allenspach Karin1

Affiliation:

1. University of Georgia College of Veterinary Medicine

2. Iowa State University

3. Ceva Santé Animale

4. University of Alberta

5. Texas A&M University

6. University of Murcia

7. Université de Lorraine, CHRU Nancy, FCRIN INI-CRCT

8. University of Glasgow

Abstract

Abstract

Background and Purpose Cardiovascular-kidney-metabolic health reflects the interactions between metabolic risk factors, chronic kidney disease, and the cardiovascular system. A growing body of literature suggests that metabolic syndrome (MetS) in individuals of normal weight is associated with a high prevalence of cardiovascular diseases and an increased mortality. The aim of this study was to establish a non-invasive preclinical model of MetS in support of future research focusing on the effects of novel antidiabetic therapies beyond glucose reduction, independent of obesity. Experimental Approach Eighteen healthy adult Beagle dogs were fed an isocaloric Western diet (WD) for ten weeks. Biospecimens were collected at baseline (BAS1) and after ten weeks of WD feeding (BAS2) for measurement of blood pressure (BP), serum chemistry, lipoprotein profiling, blood glucose, glucagon, insulin secretion, NT-proBNP, angiotensins, oxidative stress biomarkers, serum, urine, and fecal metabolomics. Differences between BAS1and BAS2 were analyzed using non-parametric Wilcoxon signed-rank testing. Key Results The isocaloric WD model induced significant variations in several markers of MetS, including elevated BP, increased glucose concentrations, and reduced HDL-cholesterol. It also caused an increase in circulating NT-proBNP levels, a decrease in serum bicarbonate, and significant changes in general metabolism, lipids, and biogenic amines. Conclusions and Implications Short-term, isocaloric feeding with a WD in dogs replicated key biological features of MetS while also causing low-grade metabolic acidosis and elevating natriuretic peptides. These findings support the use of the WD canine model for studying the metabolic effects of new antidiabetic therapies independent of obesity.

Publisher

Springer Science and Business Media LLC

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