[PDF][PDF] Disconnecting mitochondrial content from respiratory chain capacity in PGC-1-deficient skeletal muscle

GC Rowe, IS Patten, ZK Zsengeller, R El-Khoury… - Cell reports, 2013 - cell.com
GC Rowe, IS Patten, ZK Zsengeller, R El-Khoury, M Okutsu, S Bampoh, N Koulisis, C Farrell…
Cell reports, 2013cell.com
The transcriptional coactivators PGC-1α and PGC-1β are widely thought to be required for
mitochondrial biogenesis and fiber typing in skeletal muscle. Here, we show that mice
lacking both PGC-1s in myocytes do indeed have profoundly deficient mitochondrial
respiration but, surprisingly, have preserved mitochondrial content, isolated muscle
contraction capacity, fiber-type composition, in-cage ambulation, and voluntary running
capacity. Most of these findings are recapitulated in cell culture and, thus, are cell …
Summary
The transcriptional coactivators PGC-1α and PGC-1β are widely thought to be required for mitochondrial biogenesis and fiber typing in skeletal muscle. Here, we show that mice lacking both PGC-1s in myocytes do indeed have profoundly deficient mitochondrial respiration but, surprisingly, have preserved mitochondrial content, isolated muscle contraction capacity, fiber-type composition, in-cage ambulation, and voluntary running capacity. Most of these findings are recapitulated in cell culture and, thus, are cell autonomous. Functional electron microscopy reveals normal cristae density with decreased cytochrome oxidase activity. These data lead to the following surprising conclusions: (1) PGC-1s are in fact dispensable for baseline muscle function, mitochondrial content, and fiber typing, (2) endurance fatigue at low workloads is not limited by muscle mitochondrial capacity, and (3) mitochondrial content and cristae density can be dissociated from respiratory capacity.
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