The ubiquitin–proteasome system and skeletal muscle wasting

Author:

Attaix Didier1,Ventadour Sophie1,Codran Audrey1,Béchet Daniel1,Taillandier Daniel1,Combaret Lydie1

Affiliation:

1. Human Nutrition Research Centre of Clermont-Ferrand and INRA, Nutrition and Protein Metabolism Unit, 63122 Ceyrat, France

Abstract

The ubiquitin–proteasome system (UPS) is believed to degrade the major contractile skeletal muscle proteins and plays a major role in muscle wasting. Different and multiple events in the ubiquitination, deubiquitination and proteolytic machineries are responsible for the activation of the system and subsequent muscle wasting. However, other proteolytic enzymes act upstream (possibly m-calpain, cathepsin L, and/or caspase 3) and downstream (tripeptidyl-peptidase II and aminopeptidases) of the UPS, for the complete breakdown of the myofibrillar proteins into free amino acids. Recent studies have identified a few critical proteins that seem necessary for muscle wasting {i.e. the MAFbx (muscle atrophy F-box protein, also called atrogin-1) and MuRF-1 [muscle-specific RING (really interesting new gene) finger 1] ubiquitin–protein ligases}. The characterization of their signalling pathways is leading to new pharmacological approaches that can be useful to block or partially prevent muscle wasting in human patients.

Publisher

Portland Press Ltd.

Subject

Molecular Biology,Biochemistry

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