Adverse cardiac remodeling augments adipose tissue ß-adrenergic signaling and lipolysis counteracting diet-induced obesity

Adverse cardiac remodeling augments adipose tissue ß-adrenergic signaling and lipolysis counteracting diet-induced obesity

Cardiac triacylglycerol accumulation is a common characteristic of obesity and type 2 diabetes and strongly correlates with heart morbidity and mortality. We have previously shown that cardiomyocyte-specific perilipin 5 overexpression (Plin5-Tg) provokes significant cardiac steatosis via lowering ca...

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Veröffentlicht in:The Journal of biological chemistry 2023-06, Vol.299 (6), p.104788, Article 104788
Hauptverfasser: Kolleritsch, Stephanie, Pajed, Laura, Tilp, Anna, Hois, Victoria, Pototschnig, Isabella, Kien, Benedikt, Diwoky, Clemens, Hoefler, Gerald, Schoiswohl, Gabriele, Haemmerle, Guenter
Format: Artikel
Sprache:eng
Schlagworte:
adipose tissue
Adipose Tissue - metabolism
Animals
cardiac hypertrophy
Diabetes Mellitus, Type 2 - metabolism
Diet, High-Fat - adverse effects
Fatty Acids - metabolism
Heart Diseases - etiology
Heart Diseases - metabolism
Lipolysis
Mice
Mice, Transgenic
Myocytes, Cardiac - metabolism
Obesity - etiology
Obesity - metabolism
Perilipin 5
Perilipin-5 - metabolism
Receptors, Adrenergic - metabolism
thermogenesis
Triglycerides - metabolism
Ventricular Remodeling
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Zusammenfassung:Cardiac triacylglycerol accumulation is a common characteristic of obesity and type 2 diabetes and strongly correlates with heart morbidity and mortality. We have previously shown that cardiomyocyte-specific perilipin 5 overexpression (Plin5-Tg) provokes significant cardiac steatosis via lowering cardiac lipolysis and fatty acid (FA) oxidation. In strong contrast to cardiac steatosis and lethal heart dysfunction in adipose triglyceride lipase deficiency, Plin5-Tg mice do not develop heart dysfunction and show a normal life span on chow diet. This finding prompted us to study heart function and energy metabolism in Plin5-Tg mice fed high-fat diet (HFD). Plin5-Tg mice showed adverse cardiac remodeling on HFD with heart function only being compromised in one-year-old mice, likely due to reduced cardiac FA uptake, thereby delaying deleterious cardiac lipotoxicity. Notably, Plin5-Tg mice were less obese and protected from glucose intolerance on HFD. Changes in cardiac energy catabolism in Plin5-Tg mice increased ß-adrenergic signaling, lipolytic, and thermogenic protein expression in adipose tissue ultimately counteracting HFD-induced obesity. Acute cold exposure further augmented ß-adrenergic signaling in Plin5-Tg mice, whereas housing at thermoneutrality did not protect Plin5-Tg mice from HFD-induced obesity albeit blood glucose and insulin levels remained low in transgenic mice. Overall, our data suggest that the limited capacity for myocardial FA oxidation on HFD increases cardiac stress in Plin5-Tg mice, thereby stimulating adipose tissue ß-adrenergic signaling, triacylglycerol catabolism, and thermogenesis. However, long-term HFD-mediated metabolic stress causes contractile dysfunction in Plin5-Tg mice, which emphasizes the importance of a carefully controlled dietary regime in patients with cardiac steatosis and hypertrophy.
ISSN:0021-9258
1083-351X
1083-351X
DOI:10.1016/j.jbc.2023.104788