Acquisition of neural fate by combination of BMP blockade and chromatin modification
Neural induction is a process where naive cells are converted into committed cells with neural characteristics, and it occurs at the earliest step during embryogenesis. Although the signaling molecules and chromatin remodeling for neural induction have been identified, the mutual relationships betwe...
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Veröffentlicht in: | iScience 2023-10, Vol.26 (10), p.107887-107887, Article 107887 |
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Zusammenfassung: | Neural induction is a process where naive cells are converted into committed cells with neural characteristics, and it occurs at the earliest step during embryogenesis. Although the signaling molecules and chromatin remodeling for neural induction have been identified, the mutual relationships between these molecules are yet to be fully understood.
By taking advantage of the neural differentiation system of mouse embryonic stem (ES) cells, we discovered that the BMP signal regulates the expression of several polycomb repressor complex (PRC) component genes. We particularly focused on Polyhomeotic Homolog 1 (Phc1) and established Phc1-knockout (Phc1-KO) ES cells. We found that Phc1-KO failed to acquire the neural fate, and the cells remained in pluripotent or primitive non-neural states. Chromatin accessibility analysis suggests that Phc1 is essential for chromatin packing. Aberrant upregulation of the BMP signal was confirmed in the Phc1 homozygotic mutant embryos. Taken together, Phc1 is required for neural differentiation through epigenetic modification.
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•The Phc1 expression is regulated by BMP•Phc1 is required to promote in vitro neural differentiation•The chromatin loci at pluripotent genes remain poised in the absence of Phc1•Phc1 is essential for D-V patterning of eye development in mice
Epigenetics; Molecular biology; Neuroscience; Stem cells research; Transcriptomics |
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ISSN: | 2589-0042 2589-0042 |
DOI: | 10.1016/j.isci.2023.107887 |