Authors
Phil Arnold, Anne Schöler, Mikhail Pachkov, Piotr J Balwierz, Helle Jørgensen, Michael B Stadler, Erik van Nimwegen, Dirk Schübeler
Publication date
2013/1/1
Journal
Genome research
Volume
23
Issue
1
Pages
60-73
Publisher
Cold Spring Harbor Lab
Description
Although changes in chromatin are integral to transcriptional reprogramming during cellular differentiation, it is currently unclear how chromatin modifications are targeted to specific loci. To systematically identify transcription factors (TFs) that can direct chromatin changes during cell fate decisions, we model the relationship between genome-wide dynamics of chromatin marks and the local occurrence of computationally predicted TF binding sites. By applying this computational approach to a time course of Polycomb-mediated H3K27me3 marks during neuronal differentiation of murine stem cells, we identify several motifs that likely regulate the dynamics of this chromatin mark. Among these, the sites bound by REST and by the SNAIL family of TFs are predicted to transiently recruit H3K27me3 in neuronal progenitors. We validate these predictions experimentally and show that absence of REST indeed causes loss …
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