REST selectively represses a subset of RE1-containing neuronal genes in mouse embryonic stem cells

doi:10.1242/dev.028548

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First published online February 6, 2009
doi: 10.1242/10.1242/dev.028548

Development 136, 715-721 (2009)
Published by The Company of Biologists 2009

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Research Report

REST selectively represses a subset of RE1-containing neuronal genes in mouse embryonic stem cells

Helle F. Jørgensen¹^,*, Anna Terry¹, Chiara Beretta¹, C. Filipe Pereira¹, Marion Leleu¹, Zhou-Feng Chen², Claire Kelly¹, Matthias Merkenschlager¹ and Amanda G. Fisher¹^,*

¹ MRC Clinical Sciences Centre, Imperial College School of Medicine, Hammersmith Hospital Campus, Du Cane Road, London W12 0NN, UK.
² Departments of Anesthesiology, Psychiatry, Developmental Biology, Washington University School of Medicine Pain Center, St Louis, MO 63110, USA.

^* Authors for correspondence (e-mails: helle.jorgensen{at}csc.mrc.ac.uk; amanda.fisher{at}csc.mrc.ac.uk)

Accepted 5 January 2009

SUMMARY

REST is a transcriptional repressor that targets a group ofneuronal genes in non-neuronal cells. In embryonic stem (ES)cells, REST has been implicated in controlling the expressionof transcription factor genes that are crucial for lineage determinationand for maintaining ES cell potential. Here, we asked whetherREST directly regulates neural-specifying genes in mouse ES cellsusing siRNA-mediated REST knockdown and ES cells that lack functional RESTprotein as a result of gene targeting. Loss of REST did notaffect the expression of any of ten transcription factor genesknown to promote neural commitment and did not affect the expressionof several microRNAs, including miR-21, a putative REST targetin ES cells. REST-deficient ES cells retained the ability toself-renew and to undergo appropriate differentiation towardsmesoderm, endoderm and ectoderm lineages upon LIF withdrawal. Genome-wideexpression profiling showed that genes that were deregulatedin the absence of REST were preferentially expressed in thebrain and highly enriched for the presence of canonical RESTbinding sites (RE1). Chromatin immunoprecipitation studies confirmedthese genes as direct targets of REST in ES cells. Collectively,these data show that REST selectively silences a cohort of neuronalgenes in ES cells.

Key words: REST (NRSF), Embryonic stem cells, Gene silencing, Neurogenesis

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H. F. Jorgensen, A. Terry, C. Beretta, C. F. Pereira, M. Leleu, Z.-F. Chen, C. Kelly, M. Merkenschlager, and A. G. Fisher
REST selectively represses a subset of RE1-containing neuronal genes in mouse embryonic stem cells
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