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- Title
Scriptaid enhances skeletal muscle insulin action and cardiac function in obese mice.
- Authors
Gaur, Vidhi; Connor, Timothy; Venardos, Kylie; Henstridge, Darren C.; Martin, Sheree D.; Swinton, Courtney; Morrison, Shona; Aston‐Mourney, Kathryn; Gehrig, Stefan M.; van Ewijk, Roelof; Lynch, Gordon S.; Febbraio, Mark A.; Steinberg, Gregory R.; Hargreaves, Mark; Walder, Ken R.; McGee, Sean L.
- Abstract
Aim To determine the effect of Scriptaid, a compound that can replicate aspects of the exercise adaptive response through disruption of the class IIa histone deacetylase ( HDAC) corepressor complex, on muscle insulin action in obesity. Materials and methods Diet-induced obese mice were administered Scriptaid (1 mg/kg) via daily intraperitoneal injection for 4 weeks. Whole-body and skeletal muscle metabolic phenotyping of mice was performed, in addition to echocardiography, to assess cardiac morphology and function. Results Scriptaid treatment had no effect on body weight or composition, but did increase energy expenditure, supported by increased lipid oxidation, while food intake was also increased. Scriptaid enhanced the expression of oxidative genes and proteins, increased fatty acid oxidation and reduced triglycerides and diacylglycerides in skeletal muscle. Furthermore, ex vivo insulin-stimulated glucose uptake by skeletal muscle was enhanced. Surprisingly, heart weight was reduced in Scriptaid-treated mice and was associated with enhanced expression of genes involved in oxidative metabolism in the heart. Scriptaid also improved indices of both diastolic and systolic cardiac function. Conclusion These data show that pharmacological targeting of the class IIa HDAC corepressor complex with Scriptaid could be used to enhance muscle insulin action and cardiac function in obesity.
- Subjects
HISTONE deacetylase inhibitors; PHYSIOLOGICAL effects of insulin; OBESITY; HEART function tests; SKELETAL muscle physiology
- Publication
Diabetes, Obesity & Metabolism, 2017, Vol 19, Issue 7, p936
- ISSN
1462-8902
- Publication type
Article
- DOI
10.1111/dom.12896