Failures of nerve regeneration caused by aging or chronic denervation are rescued by restoring Schwann cell c-Jun.
Laura J WagstaffJosé Antonio Gómez-SánchezShaline V FazalGeorg W OttoAlastair M KilpatrickKirolos MichaelLiam YN WongKi H MaMark TurmaineJohn SvarenTessa GordonPeter Arthur-FarrajSergio Velasco-AvilesHugo CabedoCristina BenitoRhona MirskyKristjan R JessenPublished in: eLife (2021)
After nerve injury, myelin and Remak Schwann cells reprogram to repair cells specialized for regeneration. Normally providing strong regenerative support, these cells fail in aging animals, and during chronic denervation that results from slow axon growth. This impairs axonal regeneration and causes significant clinical problems. In mice, we find that repair cells express reduced c-Jun protein as regenerative support provided by these cells declines during aging and chronic denervation. In both cases, genetically restoring Schwann cell c-Jun levels restores regeneration to control levels. We identify potential gene candidates mediating this effect and implicate Shh in the control of Schwann cell c-Jun levels. This establishes that a common mechanism, reduced c-Jun in Schwann cells, regulates success and failure of nerve repair both during aging and chronic denervation. This provides a molecular framework for addressing important clinical problems, suggesting molecular pathways that can be targeted to promote repair in the PNS.
Keyphrases
- induced apoptosis
- stem cells
- cell cycle arrest
- mental health
- single cell
- cell death
- metabolic syndrome
- oxidative stress
- signaling pathway
- adipose tissue
- type diabetes
- skeletal muscle
- spinal cord injury
- palliative care
- bone marrow
- gene expression
- risk assessment
- insulin resistance
- pi k akt
- single molecule
- transcription factor
- copy number
- drug induced
- binding protein