Publication | Closed Access
Multifaceted SOX2-chromatin interaction underpins pluripotency progression in early embryos
36
Citations
65
References
2023
Year
Early EmbryosEpigeneticsEmbryologyGene ExpressionCell BiologyChromatin FunctionPluripotency RegulationPioneer Transcription FactorsChromatinLineage PlasticityInduced Pluripotent Stem CellDevelopmental BiologyChromatin StructureChromatin RemodelingNatural SciencesCell Fate DeterminationSystems BiologyMedicineEmbryonic Stem CellE3.5 Icm
Pioneer transcription factors (TFs), such as OCT4 and SOX2, play crucial roles in pluripotency regulation. However, the master TF-governed pluripotency regulatory circuitry was largely inferred from cultured cells. In this work, we investigated SOX2 binding from embryonic day 3.5 (E3.5) to E7.5 in the mouse. In E3.5 inner cell mass (ICM), SOX2 regulates the ICM-trophectoderm program but is dispensable for opening global enhancers. Instead, SOX2 occupies preaccessible enhancers in part opened by early-stage expressing TFs TFAP2C and NR5A2. SOX2 then widely redistributes when cells adopt naive and formative pluripotency by opening enhancers or poising them for rapid future activation. Hence, multifaceted pioneer TF-enhancer interaction underpins pluripotency progression in embryos, including a distinctive state in E3.5 ICM that bridges totipotency and pluripotency.
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