Extensive SUMO Modification of Repressive Chromatin Factors Distinguishes Pluripotent from Somatic Cells.

Cell Rep

Nuclear Organization and Oncogenesis Unit, Institut Pasteur, Équipe Labellisée Ligue Nationale Contre le Cancer, 75015 Paris, France; INSERM, U993, 75015 Paris, France. Electronic address:

Published: September 2020

AI Article Synopsis

  • SUMO plays a crucial role in maintaining cell identity by regulating different cellular states in mouse embryonic fibroblasts (MEFs) and embryonic stem cells (ESCs).
  • In MEFs, SUMO modifications hinder the reprogramming to pluripotency, while in ESCs, they prevent the formation of totipotent-like cells by targeting specific proteins.
  • Using mass spectrometry, the study found that the SUMOylomes of MEFs and ESCs are composed of different substrates, influencing processes like splicing and chromatin modification to control cell fate during embryonic development.

Article Abstract

Post-translational modification by SUMO is a key regulator of cell identity. In mouse embryonic fibroblasts (MEFs), SUMO impedes reprogramming to pluripotency, while in embryonic stem cells (ESCs), it represses the emergence of totipotent-like cells, suggesting that SUMO targets distinct substrates to preserve somatic and pluripotent states. Using MS-based proteomics, we show that the composition of endogenous SUMOylomes differs dramatically between MEFs and ESCs. In MEFs, SUMO2/3 targets proteins associated with canonical SUMO functions, such as splicing, and transcriptional regulators driving somatic enhancer selection. In contrast, in ESCs, SUMO2/3 primarily modifies highly interconnected repressive chromatin complexes, thereby preventing chromatin opening and transitioning to totipotent-like states. We also characterize several SUMO-modified pluripotency factors and show that SUMOylation of Dppa2 and Dppa4 impedes the conversion to 2-cell-embryo-like states. Altogether, we propose that rewiring the repertoire of SUMO target networks is a major driver of cell fate decision during embryonic development.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC7495044PMC
http://dx.doi.org/10.1016/j.celrep.2020.108146DOI Listing

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