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REST–Mediated Recruitment of Polycomb Repressor Complexes in Mammalian Cells


ABSTRACT: Genome-wide analysis of REST and Polycomb binding in Rest-/- and Eed-/- mouse embryonic stem (mES) cells showed that Rest was required for PRC1 recruitment to a subset of Polycomb regulated neuronal genes. Furthermore, we found that PRC1 can be recruited to Rest binding sites independently of CpG islands and the H3K27Me3 mark., and that PRC2 was frequently increased around Rest binding sites located in CpG-rich regions in the Rest2/2 mES cells. Published here: PLoS Genet 8(3): e1002494. doi:10.1371/journal.pgen.1002494 Examination of REST and Polycomb binding in Rest-/-, Eed-/-, and wt mES cells using ChIP-sequencing. Submitter cannot locate the raw data for GSM1169003, GSM1169004, GSM1169011, GSM1169012, GSM1169015, and GSM1169016.

ORGANISM(S): Mus musculus

SUBMITTER: Mads Lerdrup 

PROVIDER: E-GEOD-48122 | biostudies-arrayexpress |

REPOSITORIES: biostudies-arrayexpress

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Publications

REST-mediated recruitment of polycomb repressor complexes in mammalian cells.

Dietrich Nikolaj N   Lerdrup Mads M   Landt Eskild E   Agrawal-Singh Shuchi S   Bak Mads M   Tommerup Niels N   Rappsilber Juri J   Södersten Erik E   Hansen Klaus K  

PLoS genetics 20120301 3


Polycomb Repressive Complex (PRC) 1 and PRC2 regulate genes involved in differentiation and development. However, the mechanism for how PRC1 and PRC2 are recruited to genes in mammalian cells is unclear. Here we present evidence for an interaction between the transcription factor REST, PRC1, and PRC2 and show that RNF2 and REST co-regulate a number of neuronal genes in human teratocarcinoma cells (NT2-D1). Using NT2-D1 cells as a model of neuronal differentiation, we furthermore showed that reti  ...[more]

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