| Literature DB >> 25738455 |
Arieh Moussaieff1, Matthieu Rouleau2, Daniel Kitsberg3, Merav Cohen3, Gahl Levy4, Dinorah Barasch5, Alina Nemirovski5, Shai Shen-Orr6, Ilana Laevsky6, Michal Amit6, David Bomze3, Bénédicte Elena-Herrmann7, Tali Scherf8, Malka Nissim-Rafinia9, Stefan Kempa10, Joseph Itskovitz-Eldor6, Eran Meshorer9, Daniel Aberdam11, Yaakov Nahmias12.
Abstract
Loss of pluripotency is a gradual event whose initiating factors are largely unknown. Here we report the earliest metabolic changes induced during the first hours of differentiation. High-resolution NMR identified 44 metabolites and a distinct metabolic transition occurring during early differentiation. Metabolic and transcriptional analyses showed that pluripotent cells produced acetyl-CoA through glycolysis and rapidly lost this function during differentiation. Importantly, modulation of glycolysis blocked histone deacetylation and differentiation in human and mouse embryonic stem cells. Acetate, a precursor of acetyl-CoA, delayed differentiation and blocked early histone deacetylation in a dose-dependent manner. Inhibitors upstream of acetyl-CoA caused differentiation of pluripotent cells, while those downstream delayed differentiation. Our results show a metabolic switch causing a loss of histone acetylation and pluripotent state during the first hours of differentiation. Our data highlight the important role metabolism plays in pluripotency and suggest that a glycolytic switch controlling histone acetylation can release stem cells from pluripotency.Entities:
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Year: 2015 PMID: 25738455 DOI: 10.1016/j.cmet.2015.02.002
Source DB: PubMed Journal: Cell Metab ISSN: 1550-4131 Impact factor: 27.287