Skeletal muscle hypertrophy and atrophy signaling pathways

DJ Glass - The international journal of biochemistry & cell biology, 2005 - Elsevier
The international journal of biochemistry & cell biology, 2005Elsevier
Skeletal muscle hypertrophy is defined as an increase in muscle mass, which in the adult
animal comes as a result of an increase in the size, as opposed to the number, of pre-
existing skeletal muscle fibers. The protein growth factor insulin-like growth factor 1 (IGF-1)
has been demonstrated to be sufficient to induce skeletal muscle hypertrophy. Over the past
few years, signaling pathways which are activated by IGF-1, and which are responsible for
regulating protein synthesis pathways, have been defined. More recently, it has been show …
Skeletal muscle hypertrophy is defined as an increase in muscle mass, which in the adult animal comes as a result of an increase in the size, as opposed to the number, of pre-existing skeletal muscle fibers. The protein growth factor insulin-like growth factor 1 (IGF-1) has been demonstrated to be sufficient to induce skeletal muscle hypertrophy. Over the past few years, signaling pathways which are activated by IGF-1, and which are responsible for regulating protein synthesis pathways, have been defined. More recently, it has been show that IGF-1 can also block the transcriptional upregulation of key mediators of skeletal muscle atrophy, the ubiquitin-ligases MuRF1 and MAFbx (also called Atrogin-1). Further, it has been demonstrated recently that activation of the NF-κB transcription pathway, activated by cachectic factors such as TNFα, is sufficient to induce skeletal muscle atrophy, and this atrophy occurs in part via NF-κB-mediated upregulation of MuRF1. Further work has demonstrated a trigger for MAFbx expression upon treatment with TNFα—the p38 MAPK pathway. This review will focus on the recent progress in the understanding of molecular signalling, which governs skeletal muscle atrophy and hypertrophy, and the known instances of cross-regulation between the two systems.
Elsevier