Epigenetic and transcriptional regulations prime cell fate before division during human pluripotent stem cell differentiation

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作者
Pedro Madrigal
Siwei Deng
Yuliang Feng
Stefania Militi
Kim Jee Goh
Reshma Nibhani
Rodrigo Grandy
Anna Osnato
Daniel Ortmann
Stephanie Brown
Siim Pauklin
机构
[1] University of Cambridge,Department of Surgery
[2] Wellcome Genome Campus,Wellcome Sanger Institute
[3] University of Cambridge,Wellcome – MRC Cambridge Stem Cell Institute
[4] University of Oxford,Botnar Research Centre, Nuffield Department of Orthopaedics, Rheumatology and Musculoskeletal Sciences, Old Road
[5] Headington,European Molecular Biology Laboratory
[6] European Bioinformatics Institute,undefined
[7] The Francis Crick Institute,undefined
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Stem cells undergo cellular division during their differentiation to produce daughter cells with a new cellular identity. However, the epigenetic events and molecular mechanisms occurring between consecutive cell divisions have been insufficiently studied due to technical limitations. Here, using the FUCCI reporter we developed a cell-cycle synchronised human pluripotent stem cell (hPSC) differentiation system for uncovering epigenome and transcriptome dynamics during the first two divisions leading to definitive endoderm. We observed that transcription of key differentiation markers occurs before cell division, while chromatin accessibility analyses revealed the early inhibition of alternative cell fates. We found that Activator protein-1 members controlled by p38/MAPK signalling are necessary for inducing endoderm while blocking cell fate shifting toward mesoderm, and that enhancers are rapidly established and decommissioned between different cell divisions. Our study has practical biomedical utility for producing hPSC-derived patient-specific cell types since p38/MAPK induction increased the differentiation efficiency of insulin-producing pancreatic beta-cells.
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