Litcius/Paper detail

Supraphysiological activation of TAK1 promotes skeletal muscle growth and mitigates neurogenic atrophy

Anirban Roy, Ashok Kumar

2022Nature Communications29 citationsDOIOpen Access PDF

Abstract

Skeletal muscle mass is regulated through coordinated activation of multiple signaling pathways. TAK1 signalosome has been found to be activated in various conditions of muscle atrophy and hypertrophy. However, the role and mechanisms by which TAK1 regulates skeletal muscle mass remain less understood. Here, we demonstrate that supraphysiological activation of TAK1 in skeletal muscle of adult mice stimulates translational machinery, protein synthesis, and myofiber growth. TAK1 causes phosphorylation of elongation initiation factor 4E (eIF4E) independent of mTOR. Inactivation of TAK1 disrupts neuromuscular junction morphology and causes deregulation of Smad signaling. Using genetic approaches, we demonstrate that TAK1 prevents excessive loss of muscle mass during denervation. TAK1 favors the nuclear translocation of Smad4 and cytoplasmic retention of Smad6. TAK1 is also required for the phosphorylation of eIF4E in denervated skeletal muscle. Collectively, our results demonstrate that TAK1 supports skeletal muscle growth and prevents neurogenic muscle atrophy in adult mice.

Topics & Concepts

Skeletal muscleMuscle hypertrophyMyostatinDenervationMuscle atrophyPhosphorylationCell biologyAtrophyMyocyteSarcopeniaBiologySignal transductionEndocrinologyChemistryInternal medicineMedicineMuscle Physiology and DisordersCardiomyopathy and Myosin StudiesNeurogenetic and Muscular Disorders Research