Transcriptional coactivator PGC-1α controls the energy state and contractile function of cardiac muscle
2005; Cell Press; Volume: 1; Issue: 4 Linguagem: Inglês
10.1016/j.cmet.2005.03.002
ISSN1932-7420
AutoresZoltàn Arany, Huamei He, Jiandie D. Lin, Kirsten Hoyer, Christoph Handschin, Okan Toka, Ferhaan Ahmad, Takashi Matsui, Sherry Chin, Pei-Hsuan Wu, Igor I. Rybkin, John M. Shelton, Monia Manieri, Saverio Cinti, Frederick J. Schöen, Rhonda Bassel‐Duby, Anthony Rosenzweig, Joanne S. Ingwall, Bruce M. Spiegelman,
Tópico(s)Metabolism, Diabetes, and Cancer
ResumoSummary Skeletal and cardiac muscle depend on high turnover of ATP made by mitochondria in order to contract efficiently. The transcriptional coactivator PGC-1α has been shown to function as a major regulator of mitochondrial biogenesis and respiration in both skeletal and cardiac muscle, but this has been based only on gain-of-function studies. Using genetic knockout mice, we show here that, while PGC-1α KO mice appear to retain normal mitochondrial volume in both muscle beds, expression of genes of oxidative phosphorylation is markedly blunted. Hearts from these mice have reduced mitochondrial enzymatic activities and decreased levels of ATP. Importantly, isolated hearts lacking PGC-1α have a diminished ability to increase work output in response to chemical or electrical stimulation. As mice lacking PGC-1α age, cardiac dysfunction becomes evident in vivo. These data indicate that PGC-1α is vital for the heart to meet increased demands for ATP and work in response to physiological stimuli.
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