eIF2B localization and its regulation during the integrated stress response is cell-type specific

HANSON, Filipe, RIBEIRO DE OLIVEIRA, Madalena, CROSS, Alison, ALLEN, Liz and CAMPBELL, Susan (2024). eIF2B localization and its regulation during the integrated stress response is cell-type specific. iScience, 27 (9): 110851. [Article]

Documents
34196:680104
[thumbnail of Hanson-eIF2BLocalizationRegulation(VoR).pdf]
Preview
PDF
Hanson-eIF2BLocalizationRegulation(VoR).pdf - Published Version
Available under License Creative Commons Attribution.

Download (7MB) | Preview
Abstract
Eukaryotic initiation factor 2B (eIF2B) controls translation initiation by recycling inactive eIF2-GDP to active eIF2-GTP. Under cellular stress, the integrated stress response (ISR) is activated inhibiting eIF2B activity resulting in the translation attenuation and reprogramming of gene expression to overcome the stress. The ISR can dictate cell fate wherein chronic activation has pathological outcomes. Vanishing white matter disease (VWMD) is a chronic ISR-related disorder with mutations in eIF2B targeting astrocyte and oligodendrocyte cells. Regulation of eIF2B localization (eIF2B bodies) has been implicated in the ISR. We present evidence that neuronal and glial cell types possess distinct patterns of eIF2B bodies which change in a manner correlating to acute and chronic ISR activation. We also demonstrate that while neural and glial cell types respond similarly to the acute induction of the ISR a chronic ISR exerts cell-type specific differences. These findings provide key insights into neural cell responses and adaptation to cellular stress.
More Information
Statistics

Downloads

Downloads per month over past year

View more statistics

Metrics

Altmetric Badge

Dimensions Badge

Share
Add to AnyAdd to TwitterAdd to FacebookAdd to LinkedinAdd to PinterestAdd to Email

Actions (login required)

View Item View Item