Publication | Open Access
Cell Signaling Coordinates Global PRC2 Recruitment and Developmental Gene Expression in Murine Embryonic Stem Cells
14
Citations
44
References
2020
Year
Developmental Gene ExpressionCell SpecializationEpigeneticsTranscriptional RegulationSignaling PathwayGene PromotersNaive MescsStem CellsCell SignalingMolecular SignalingGene ExpressionEpigenetic RegulationCell BiologyTranscription RegulationCell LineageLineage PlasticityDevelopmental BiologyNatural SciencesGene RegulationStem Cell ResearchCell Fate DeterminationSystems BiologyMedicineEmbryonic Stem Cell
The recruitment of Polycomb repressive complex 2 (PRC2) to gene promoters is critical for its function in repressing gene expression in murine embryonic stem cells (mESCs). However, previous studies have demonstrated that although the expression of early lineage-specific genes is largely repressed, the genome-wide PRC2 occupancy is unexpectedly reduced in naive mESCs. In this study, we provide evidence that fibroblast growth factor/extracellular signal-regulated kinase signaling determines the global PRC2 occupancy through regulating the expression of PRC2-recruiting factor JARID2 in naive mESCs. At the transcriptional level, the de-repression of bivalent genes is predominantly determined by the presence of cell signaling-associated transcription factors but not the status of PRC2 occupancy at gene promoters. Hence, this study not only reveals a key molecular mechanism by which cell signaling regulates the PRC2 occupancy in mESCs but also elucidates the functional roles of transcription factors and Polycomb-mediated epigenetic mechanisms in transcriptional regulation.
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