Zeb2 Recruits HDAC-NuRD to Inhibit Notch and Controls Schwann Cell Differentiation and Remyelination

The mechanisms that coordinate and balance a complex network of opposing regulators to control Schwann cell (SC) differentiation remain elusive. Here we demonstrate that zinc-finger E-box binding-homeobox 2 (Zeb2/Sip1) transcription factor is a critical intrinsic timer that controls the onset of Sch...

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Autores principales: Wu, Lai Man Natalie, Wang, Jincheng, Conidi, Andrea, Zhao, Chuntao, Wang, Haibo, Ford, Zachary, Zhang, Liguo, Zweier, Christiane, Ayee, Brian G., Maurel, Patrice, Zwijsen, An, Chan, Jonah R., Jankowski, Michael P., Huylebroeck, Danny, Lu, Q. Richard
Formato: Online Artículo Texto
Lenguaje:English
Publicado: 2016
Materias:
Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4961522/
https://www.ncbi.nlm.nih.gov/pubmed/27294509
http://dx.doi.org/10.1038/nn.4322
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author Wu, Lai Man Natalie
Wang, Jincheng
Conidi, Andrea
Zhao, Chuntao
Wang, Haibo
Ford, Zachary
Zhang, Liguo
Zweier, Christiane
Ayee, Brian G.
Maurel, Patrice
Zwijsen, An
Chan, Jonah R.
Jankowski, Michael P.
Huylebroeck, Danny
Lu, Q. Richard
author_facet Wu, Lai Man Natalie
Wang, Jincheng
Conidi, Andrea
Zhao, Chuntao
Wang, Haibo
Ford, Zachary
Zhang, Liguo
Zweier, Christiane
Ayee, Brian G.
Maurel, Patrice
Zwijsen, An
Chan, Jonah R.
Jankowski, Michael P.
Huylebroeck, Danny
Lu, Q. Richard
author_sort Wu, Lai Man Natalie
collection PubMed
description The mechanisms that coordinate and balance a complex network of opposing regulators to control Schwann cell (SC) differentiation remain elusive. Here we demonstrate that zinc-finger E-box binding-homeobox 2 (Zeb2/Sip1) transcription factor is a critical intrinsic timer that controls the onset of Schwann cell (SC) differentiation by recruiting HDAC1/2-NuRD co-repressor complexes. Zeb2 deletion arrests SCs at an undifferentiated state during peripheral nerve development and inhibits remyelination after injury. Zeb2 antagonizes inhibitory effectors including Notch and Sox2. Importantly, genome-wide transcriptome analysis reveals a Zeb2 target gene, encoding the Notch effector Hey2, as a potent inhibitor for SC differentiation. Strikingly, a genetic Zeb2 variant, which is associated with Mowat-Wilson syndrome, disrupts the interaction with HDAC1/2-NuRD and abolishes Zeb2 activity for SC differentiation. Therefore, Zeb2 controls SC maturation by recruiting HDAC1/2-NuRD complexes and inhibiting a novel Notch-Hey2 signaling axis, pointing to the critical role of HDAC1/2-NuRD activity in peripheral neuropathies caused by ZEB2 mutations.
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spelling pubmed-49615222016-12-13 Zeb2 Recruits HDAC-NuRD to Inhibit Notch and Controls Schwann Cell Differentiation and Remyelination Wu, Lai Man Natalie Wang, Jincheng Conidi, Andrea Zhao, Chuntao Wang, Haibo Ford, Zachary Zhang, Liguo Zweier, Christiane Ayee, Brian G. Maurel, Patrice Zwijsen, An Chan, Jonah R. Jankowski, Michael P. Huylebroeck, Danny Lu, Q. Richard Nat Neurosci Article The mechanisms that coordinate and balance a complex network of opposing regulators to control Schwann cell (SC) differentiation remain elusive. Here we demonstrate that zinc-finger E-box binding-homeobox 2 (Zeb2/Sip1) transcription factor is a critical intrinsic timer that controls the onset of Schwann cell (SC) differentiation by recruiting HDAC1/2-NuRD co-repressor complexes. Zeb2 deletion arrests SCs at an undifferentiated state during peripheral nerve development and inhibits remyelination after injury. Zeb2 antagonizes inhibitory effectors including Notch and Sox2. Importantly, genome-wide transcriptome analysis reveals a Zeb2 target gene, encoding the Notch effector Hey2, as a potent inhibitor for SC differentiation. Strikingly, a genetic Zeb2 variant, which is associated with Mowat-Wilson syndrome, disrupts the interaction with HDAC1/2-NuRD and abolishes Zeb2 activity for SC differentiation. Therefore, Zeb2 controls SC maturation by recruiting HDAC1/2-NuRD complexes and inhibiting a novel Notch-Hey2 signaling axis, pointing to the critical role of HDAC1/2-NuRD activity in peripheral neuropathies caused by ZEB2 mutations. 2016-06-13 2016-08 /pmc/articles/PMC4961522/ /pubmed/27294509 http://dx.doi.org/10.1038/nn.4322 Text en Users may view, print, copy, and download text and data-mine the content in such documents, for the purposes of academic research, subject always to the full Conditions of use: http://www.nature.com/authors/editorial_policies/license.html#terms
spellingShingle Article
Wu, Lai Man Natalie
Wang, Jincheng
Conidi, Andrea
Zhao, Chuntao
Wang, Haibo
Ford, Zachary
Zhang, Liguo
Zweier, Christiane
Ayee, Brian G.
Maurel, Patrice
Zwijsen, An
Chan, Jonah R.
Jankowski, Michael P.
Huylebroeck, Danny
Lu, Q. Richard
Zeb2 Recruits HDAC-NuRD to Inhibit Notch and Controls Schwann Cell Differentiation and Remyelination
title Zeb2 Recruits HDAC-NuRD to Inhibit Notch and Controls Schwann Cell Differentiation and Remyelination
title_full Zeb2 Recruits HDAC-NuRD to Inhibit Notch and Controls Schwann Cell Differentiation and Remyelination
title_fullStr Zeb2 Recruits HDAC-NuRD to Inhibit Notch and Controls Schwann Cell Differentiation and Remyelination
title_full_unstemmed Zeb2 Recruits HDAC-NuRD to Inhibit Notch and Controls Schwann Cell Differentiation and Remyelination
title_short Zeb2 Recruits HDAC-NuRD to Inhibit Notch and Controls Schwann Cell Differentiation and Remyelination
title_sort zeb2 recruits hdac-nurd to inhibit notch and controls schwann cell differentiation and remyelination
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4961522/
https://www.ncbi.nlm.nih.gov/pubmed/27294509
http://dx.doi.org/10.1038/nn.4322
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