The transcriptional coregulator PGC-1β controls mitochondrial function and anti-oxidant defence in skeletal muscles

转录共调节因子 PGC-1β 控制骨骼肌的线粒体功能和抗氧化防御

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作者:Thanuja Gali Ramamoorthy, Gilles Laverny, Anna-Isabel Schlagowski, Joffrey Zoll, Nadia Messaddeq, Jean-Marc Bornert, Salvatore Panza, Arnaud Ferry, Bernard Geny, Daniel Metzger

Abstract

The transcriptional coregulators PGC-1α and PGC-1β modulate the expression of numerous partially overlapping genes involved in mitochondrial biogenesis and energetic metabolism. The physiological role of PGC-1β is poorly understood in skeletal muscle, a tissue of high mitochondrial content to produce ATP levels required for sustained contractions. Here we determine the physiological role of PGC-1β in skeletal muscle using mice, in which PGC-1β is selectively ablated in skeletal myofibres at adulthood (PGC-1β((i)skm-/-) mice). We show that myofibre myosin heavy chain composition and mitochondrial number, muscle strength and glucose homeostasis are unaffected in PGC-1β((i)skm-/-) mice. However, decreased expression of genes controlling mitochondrial protein import, translational machinery and energy metabolism in PGC-1β((i)skm-/-) muscles leads to mitochondrial structural and functional abnormalities, impaired muscle oxidative capacity and reduced exercise performance. Moreover, enhanced free-radical leak and reduced expression of the mitochondrial anti-oxidant enzyme Sod2 increase muscle oxidative stress. PGC-1β is therefore instrumental for skeletal muscles to cope with high energetic demands.

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