The microRNA cluster C19MC confers differentiation potential into trophoblast lineages upon human pluripotent stem cells

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作者
Norio Kobayashi
Hiroaki Okae
Hitoshi Hiura
Naoto Kubota
Eri H. Kobayashi
Shun Shibata
Akira Oike
Takeshi Hori
Chie Kikutake
Hirotaka Hamada
Hirokazu Kaji
Mikita Suyama
Marie-Line Bortolin-Cavaillé
Jérôme Cavaillé
Takahiro Arima
机构
[1] Tohoku University Graduate School of Medicine,Department of Informative Genetics, Environment and Genome Research Center
[2] Tokyo University of Agriculture,Department of Bioscience, Faculty of Life Science
[3] Kyushu University,Division of Bioinformatics, Medical Institute of Bioregulation
[4] Tokyo Medical and Dental University,Department of Biomechanics, Institute of Biomaterials and Bioengineering
[5] University of Toulouse,Molecular, Cellular and Developmental biology department (MCD), Centre de Biologie Intégrative (CBI)
[6] CNRS,undefined
[7] UPS,undefined
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摘要
The first cell fate commitment during mammalian development is the specification of the inner cell mass and trophectoderm. This irreversible cell fate commitment should be epigenetically regulated, but the precise mechanism is largely unknown in humans. Here, we show that naïve human embryonic stem (hES) cells can transdifferentiate into trophoblast stem (hTS) cells, but primed hES cells cannot. Our transcriptome and methylome analyses reveal that a primate-specific miRNA cluster on chromosome 19 (C19MC) is active in naïve hES cells but epigenetically silenced in primed ones. Moreover, genome and epigenome editing using CRISPR/Cas systems demonstrate that C19MC is essential for hTS cell maintenance and C19MC-reactivated primed hES cells can give rise to hTS cells. Thus, we reveal that C19MC activation confers differentiation potential into trophoblast lineages on hES cells. Our findings are fundamental to understanding the epigenetic regulation of human early development and pluripotency.
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