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  4. Somatic and axonal LIGHT signaling elicit degenerative and regenerative responses in motoneurons, respectively
 
research article

Somatic and axonal LIGHT signaling elicit degenerative and regenerative responses in motoneurons, respectively

Otsmane, Belkacem
•
Moumen, Anice
•
Aebischer, Julianne  
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2014
Embo Reports

A receptor-ligand interaction can evoke a broad range of biological activities in different cell types depending on receptor identity and cell type-specific post-receptor signaling intermediates. Here, we show that the TNF family member LIGHT, known to act as a death-triggering factor in motoneurons through LT-beta R, can also promote axon outgrowth and branching in motoneurons through the same receptor. LIGHT-induced axonal elongation and branching require ERK and caspase-9 pathways. This distinct response involves a compartment-specific activation of LIGHT signals, with somatic activation-inducing death, while axonal stimulation promotes axon elongation and branching in motoneurons. Following peripheral nerve damage, LIGHT increases at the lesion site through expression by invading B lymphocytes, and genetic deletion of Light significantly delays functional recovery. We propose that a central and peripheral activation of the LIGHT pathway elicits different functional responses in motoneurons.

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Type
research article
DOI
10.1002/embr.201337948
Web of Science ID

WOS:000335579900019

Author(s)
Otsmane, Belkacem
Moumen, Anice
Aebischer, Julianne  
Coque, Emmanuelle
Sar, Chamroeun
Sunyach, Claire
Salsac, Celine
Valmier, Jean
Salinas, Sara
Bowerman, Melissa
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Date Issued

2014

Publisher

Wiley-Blackwell

Published in
Embo Reports
Volume

15

Issue

5

Start page

540

End page

547

Subjects

motoneuron

•

axon outgrowth

•

LIGHT

•

cell death

•

branching

Editorial or Peer reviewed

REVIEWED

Written at

EPFL

EPFL units
BMI  
Available on Infoscience
June 23, 2014
Use this identifier to reference this record
https://infoscience.epfl.ch/handle/20.500.14299/104603
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