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The RNA Helicase DDX6 Controls Cellular Plasticity by Modulating P-Body Homeostasis

Authors :
Kendell Clement
Chuck Haggerty
Stefan Aigner
Hongcang Gu
Alexander Meissner
Inna Lipchina
Anthony Anselmo
Steven P. Gygi
Justin Brumbaugh
Fei Ji
John L. Pulice
Mattia F. M. Gerli
Katie J. Clowers
Aaron J. Huebner
Inés Rabano Jiménez
En-Ching Luo
Ruslan I. Sadreyev
Bruno Di Stefano
Konrad Hochedlinger
Jocelyn Charlton
Marit A.C. de Kort
Gene W. Yeo
Source :
Cell Stem Cell, Cell stem cell, vol 25, iss 5
Publication Year :
2019

Abstract

Post-transcriptional mechanisms have the potential to influence complex changes in gene expression, yet their role in cell fate transitions remains largely unexplored. Here, we show that suppression of the RNA helicase DDX6 endows human and mouse primed embryonic stem cells (ESCs) with a differentiation-resistant, "hyper-pluripotent" state, which readily reprograms to a naive state resembling the preimplantation embryo. We further demonstrate that DDX6 plays a key role in adult progenitors where it controls the balance between self-renewal and differentiation in a context-dependent manner. Mechanistically, DDX6 mediates the translational suppression of target mRNAs in P-bodies. Upon loss of DDX6 activity, P-bodies dissolve and release mRNAs encoding fate-instructive transcription and chromatin factors that re-enter the ribosome pool. Increased translation of these targets impacts cell fate by rewiring the enhancer, heterochromatin, and DNA methylation landscapes of undifferentiated cell types. Collectively, our data establish a link between P-body homeostasis, chromatin organization, and stem cell potency.

Details

ISSN :
18759777
Volume :
25
Issue :
5
Database :
OpenAIRE
Journal :
Cell stem cell
Accession number :
edsair.doi.dedup.....f897f0d3dccf74c0593b4875366ce860