Cardioprotective effects of short-term empagliflozin treatment in db/db mice

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Bernhard Radlinger
Florian Hornsteiner
Sabrina Folie
Willi Salvenmoser
Bernhard J. Haubner
Thomas Schuetz
Simone Haas
Claudia Ress
Timon E. Adolph
Karin Salzmann
Bernhard Weiss
Herbert Tilg
Susanne Kaser
机构
[1] Medical University Innsbruck,Department of Internal Medicine I, Christian Doppler Laboratory for Metabolic Crosstalk
[2] Medical University Innsbruck,Department of Internal Medicine I
[3] Leopold Franzens University Innsbruck,Insitute of Zoology and Center of Molecular Biosciences Innsbruck (CBMI)
[4] Medical University Innsbruck,Department of Internal Medicine III
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Scientific Reports | / 10卷
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Sodium glucose transporter (SGLT)-2 inhibitors have consistently shown cardioprotective effects independent of the glycemic status of treated patients. In this study we aimed to investigate underlying mechanisms of short-term empagliflozin treatment in a mouse model of type II diabetes. Male db/db mice were fed a western type diet with or without enrichment with empagliflozin for 7 days. While glucose tolerance was significantly improved in empagliflozin treated mice, body weight and fasting insulin levels were comparable in both groups. Cardiac insulin signaling activity indicated by reduced proteinkinase B (AKT) phosphorylation was significantly decreased in the empagliflozin treated group. Remarkably, mitochondrial mass estimated by citrate synthase activity was significantly elevated in empagliflozin treated mice. Accordingly, mitochondrial morphology was significantly altered upon treatment with empagliflozin as analysed by transmission electron microscopy. Additionally, short-term empagliflozin therapy was associated with a changed cardiac tissue cytokine expression in favor of an anti-inflammatory pattern. Our data suggest that early cardioprotection in empagliflozin treated mice is independent of a reduction in body weight or hyperinsulinemia. Ameliorated mitochondrial ultrastructure, attenuated cardiac insulin signaling and diminished cardiac inflammation might contribute to the cardioprotective effects of empagliflozin.
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