Inhibition of Cell Division and DNA Replication Impair Mouse-Naïve Pluripotency Exit

The cell cycle has gained attention as a key determinant for cell fate decisions, but the contribution of DNA replication and mitosis in stem cell differentiation has not been extensively studied. To understand if these processes act as “windows of opportunity” for changes in cell identity, we estab...

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Detalles Bibliográficos
Autores principales: Waisman, A., Vazquez Echegaray, C., Solari, C., Cosentino, M.S., Martyn, I., Deglincerti, A., Ozair, M.Z., Ruzo, A., Barañao, L., Miriuka, S., Brivanlou, A., Guberman, A.
Formato: JOUR
Materias:
cell division
DNA replication
mouse embryonic stem cells introduction
primitive ectoderm-like cells
DNA methyltransferase 3A
kruppel like factor 4
octamer transcription factor 6
protein p53
transcription factor NANOG
transcription factor Otx2
animal cell
Article
cell cycle
cell cycle G1 phase
cell cycle regulation
cell cycle S phase
cell differentiation
controlled study
mitosis
mouse
mouse embryonic stem cell
nonhuman
pluripotent stem cell
priority journal
stem cell
animal
genetic transcription
physiology
Animals
Cell Differentiation
Cell Division
DNA Replication
Mice
Mouse Embryonic Stem Cells
Pluripotent Stem Cells
Transcription, Genetic
Acceso en línea:http://hdl.handle.net/20.500.12110/paper_00222836_v429_n18_p2802_Waisman
Aporte de:
Biblioteca Digital - Facultad de Ciencias Exactas y Naturales (UBA) de Universidad de Buenos Aires
Descripción
Sumario:The cell cycle has gained attention as a key determinant for cell fate decisions, but the contribution of DNA replication and mitosis in stem cell differentiation has not been extensively studied. To understand if these processes act as “windows of opportunity” for changes in cell identity, we established synchronized cultures of mouse embryonic stem cells as they exit the ground state of pluripotency. We show that initial transcriptional changes in this transition do not require passage through mitosis and that conversion to primed pluripotency is linked to lineage priming in the G1 phase. Importantly, we demonstrate that impairment of DNA replication severely blocks transcriptional switch to primed pluripotency, even in the absence of p53 activity induced by the DNA damage response. Our data suggest an important role for DNA replication during mouse embryonic stem cell differentiation, which could shed light on why pluripotent cells are only receptive to differentiation signals during G1, that is, before the S phase. © 2017 Elsevier Ltd

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