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116596 |
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|a dc
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|a Sahakyan, Anna
|e author
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|a Massachusetts Institute of Technology. Department of Biology
|e contributor
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|a Jaenisch, Rudolf
|e contributor
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|a Kim, Rachel
|e author
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|a Chronis, Constantinos
|e author
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|a Sabri, Shan
|e author
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|a Bonora, Giancarlo
|e author
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|a Theunissen, Thorold W.
|e author
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|a Kuoy, Edward
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|a Langerman, Justin
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|a Clark, Amander T.
|e author
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|a Plath, Kathrin
|e author
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|a Jaenisch, Rudolf
|e author
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|a Human Naive Pluripotent Stem Cells Model X Chromosome Dampening and X Inactivation
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|b Elsevier,
|c 2018-06-26T13:29:21Z.
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|z Get fulltext
|u http://hdl.handle.net/1721.1/116596
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|a Naive human embryonic stem cells (hESCs) can be derived from primed hESCs or directly from blastocysts, but their X chromosome state has remained unresolved. Here, we show that the inactive X chromosome (Xi) of primed hESCs was reactivated in naive culture conditions. Like cells of the blastocyst, the resulting naive cells contained two active X chromosomes with XIST expression and chromosome-wide transcriptional dampening and initiated XIST-mediated X inactivation upon differentiation. Both establishment of and exit from the naive state (differentiation) happened via an XIST-negative XaXaintermediate. Together, these findings identify a cell culture system for functionally exploring the two X chromosome dosage compensation processes in early human development: X dampening and X inactivation. However, remaining differences between naive hESCs and embryonic cells related to mono-allelic XIST expression and non-random X inactivation highlight the need for further culture improvement. As the naive state resets Xiabnormalities seen in primed hESCs, it may provide cells better suited for downstream applications.
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|a Article
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|t Cell Stem Cell
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