Authors
Joaquín Pérez-Schindler, Serge Summermatter, Silvia Salatino, Francesco Zorzato, Markus Beer, Piotr J Balwierz, Erik van Nimwegen, Jérôme N Feige, Johan Auwerx, Christoph Handschin
Publication date
2012/12/15
Journal
Molecular and cellular biology
Volume
32
Issue
24
Pages
4913-4924
Publisher
American Society for Microbiology
Description
Skeletal muscle exhibits a high plasticity and accordingly can quickly adapt to different physiological and pathological stimuli by changing its phenotype largely through diverse epigenetic mechanisms. The nuclear receptor corepressor 1 (NCoR1) has the ability to mediate gene repression; however, its role in regulating biological programs in skeletal muscle is still poorly understood. We therefore studied the mechanistic and functional aspects of NCoR1 function in this tissue. NCoR1 muscle-specific knockout mice exhibited a 7.2% higher peak oxygen consumption (VO 2peak), a 11% reduction in maximal isometric force, and increased ex vivo fatigue resistance during maximal stimulation. Interestingly, global gene expression analysis revealed a high overlap between the effects of NCoR1 deletion and peroxisome proliferator-activated receptor gamma (PPARγ) coactivator 1α (PGC-1α) overexpression on oxidative …
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