Nature Communications (Oct 2024)

ZIC2 and ZIC3 promote SWI/SNF recruitment to safeguard progression towards human primed pluripotency

  • Ishtiaque Hossain,
  • Pierre Priam,
  • Sofia C. Reynoso,
  • Sahil Sahni,
  • Xiao X. Zhang,
  • Laurence Côté,
  • Joelle Doumat,
  • Candus Chik,
  • Tianxin Fu,
  • Julie A. Lessard,
  • William A. Pastor

DOI
https://doi.org/10.1038/s41467-024-52431-1
Journal volume & issue
Vol. 15, no. 1
pp. 1 – 16

Abstract

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Abstract The primed epiblast acts as a transitional stage between the relatively homogeneous naïve epiblast and the gastrulating embryo. Its formation entails coordinated changes in regulatory circuits driven by transcription factors and epigenetic modifications. Using a multi-omic approach in human embryonic stem cell models across the spectrum of peri-implantation development, we demonstrate that the transcription factors ZIC2 and ZIC3 have overlapping but essential roles in opening primed-specific enhancers. Together, they are essential to facilitate progression to and maintain primed pluripotency. ZIC2/3 accomplish this by recruiting SWI/SNF to chromatin and loss of ZIC2/3 or degradation of SWI/SNF both prevent enhancer activation. Loss of ZIC2/3 also results in transcriptome changes consistent with perturbed Polycomb activity and a shift towards the expression of genes linked to differentiation towards the mesendoderm. Additionally, we find an intriguing dependency on the transcriptional machinery for sustained recruitment of ZIC2/3 over a subset of primed-hESC specific enhancers. Taken together, ZIC2 and ZIC3 regulate highly dynamic lineage-specific enhancers and collectively act as key regulators of human primed pluripotency.