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GATA transcription factors drive initial Xist upregulation after fertilization through direct activation of long-range enhancers.


ABSTRACT: X-chromosome inactivation (XCI) balances gene expression between the sexes in female mammals. Shortly after fertilization, upregulation of Xist RNA from one X chromosome initiates XCI, leading to chromosome-wide gene silencing. XCI is maintained in all cell types, except the germ line and the pluripotent state where XCI is reversed. The mechanisms triggering Xist upregulation have remained elusive. Here we identify GATA transcription factors as potent activators of Xist. Through a pooled CRISPR activation screen in murine embryonic stem cells, we demonstrate that GATA1, as well as other GATA transcription factors can drive ectopic Xist expression. Moreover, we describe GATA-responsive regulatory elements in the Xist locus bound by different GATA factors. Finally, we show that GATA factors are essential for XCI induction in mouse preimplantation embryos. Deletion of GATA1/4/6 or GATA-responsive Xist enhancers in mouse zygotes effectively prevents Xist upregulation. We propose that the activity or complete absence of various GATA family members controls initial Xist upregulation, XCI maintenance in extra-embryonic lineages and XCI reversal in the epiblast.

SUBMITTER: Ravid Lustig L 

PROVIDER: S-EPMC10635832 | biostudies-literature | 2023 Nov

REPOSITORIES: biostudies-literature

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GATA transcription factors drive initial Xist upregulation after fertilization through direct activation of long-range enhancers.

Ravid Lustig Liat L   Sampath Kumar Abhishek A   Schwämmle Till T   Dunkel Ilona I   Noviello Gemma G   Limberg Elodie E   Weigert Raha R   Pacini Guido G   Buschow René R   Ghauri Afrah A   Stötzel Maximilian M   Wittler Lars L   Meissner Alexander A   Schulz Edda G EG  

Nature cell biology 20231106 11


X-chromosome inactivation (XCI) balances gene expression between the sexes in female mammals. Shortly after fertilization, upregulation of Xist RNA from one X chromosome initiates XCI, leading to chromosome-wide gene silencing. XCI is maintained in all cell types, except the germ line and the pluripotent state where XCI is reversed. The mechanisms triggering Xist upregulation have remained elusive. Here we identify GATA transcription factors as potent activators of Xist. Through a pooled CRISPR  ...[more]

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