Nuclear pore complex remodeling by p75(NTR) cleavage controls TGF-β signaling and astrocyte functions.

Christian SchachtrupJae Kyu RyuKönül MammadzadaAbdullah S KhanPeter Mark CarltonAlex PerezFrank ChristianNatacha Le MoanEirini VagenaBernat Baeza-RajaVictoria RafalskiJustin P ChanRoland NitschkeMiles D HouslayMark H EllismanTony Wyss-CorayJorge J PalopKaterina Akassoglou

Published in: Nature neuroscience (2015)

Astrocytes modulate neuronal activity and inhibit regeneration. We show that cleaved p75 neurotrophin receptor (p75(NTR)) is a component of the nuclear pore complex (NPC) required for glial scar formation and reduced gamma oscillations in mice via regulation of transforming growth factor (TGF)-β signaling. Cleaved p75(NTR) interacts with nucleoporins to promote Smad2 nucleocytoplasmic shuttling. Thus, NPC remodeling by regulated intramembrane cleavage of p75(NTR) controls astrocyte-neuronal communication in response to profibrotic factors.

Keyphrases

transforming growth factor
epithelial mesenchymal transition
stem cells
dna binding
cerebral ischemia
transcription factor
binding protein
signaling pathway
type diabetes
working memory
high fat diet induced
adipose tissue
metabolic syndrome
spinal cord
subarachnoid hemorrhage
brain injury
wild type