| Literature DB >> 28467934 |
Weiwei Fan1, Wanda Waizenegger1, Chun Shi Lin1, Vincenzo Sorrentino2, Ming-Xiao He1, Christopher E Wall1, Hao Li2, Christopher Liddle3, Ruth T Yu1, Annette R Atkins1, Johan Auwerx2, Michael Downes4, Ronald M Evans5.
Abstract
Management of energy stores is critical during endurance exercise; a shift in substrate utilization from glucose toward fat is a hallmark of trained muscle. Here we show that this key metabolic adaptation is both dependent on muscle PPARδ and stimulated by PPARδ ligand. Furthermore, we find that muscle PPARδ expression positively correlates with endurance performance in BXD mouse reference populations. In addition to stimulating fatty acid metabolism in sedentary mice, PPARδ activation potently suppresses glucose catabolism and does so without affecting either muscle fiber type or mitochondrial content. By preserving systemic glucose levels, PPARδ acts to delay the onset of hypoglycemia and extends running time by ∼100 min in treated mice. Collectively, these results identify a bifurcated PPARδ program that underlies glucose sparing and highlight the potential of PPARδ-targeted exercise mimetics in the treatment of metabolic disease, dystrophies, and, unavoidably, the enhancement of athletic performance.Entities:
Keywords: PPARδ; endurance exercise; exercise mimetics; fatty acid metabolism; glucose metabolism; muscle
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Year: 2017 PMID: 28467934 PMCID: PMC5492977 DOI: 10.1016/j.cmet.2017.04.006
Source DB: PubMed Journal: Cell Metab ISSN: 1550-4131 Impact factor: 27.287