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Rlim-Dependent and -Independent Pathways for X Chromosome Inactivation in Female ESCs.

Citation
Wang, F., et al. “Rlim-Dependent And -Independent Pathways For X Chromosome Inactivation In Female Escs.”. Cell Reports, pp. 3691-3699.
Author Feng Wang, Kurtis N McCannell, Ana Bošković, Xiaochun Zhu, JongDae Shin, Jun Yu, Judith Gallant, Meg Byron, Jeanne B Lawrence, Lihua J Zhu, Stephen N Jones, Oliver J Rando, Thomas G Fazzio, Ingolf Bach
Keywords EB differentiation, ESC, Rlim, Rlim-independent XCI, Rnf12, X chromosome inactivation, XCI, XCI regulation, Xist, physiological oxygen levels
Abstract

During female mouse embryogenesis, two forms of X chromosome inactivation (XCI) ensure dosage compensation from sex chromosomes. Beginning at the four-cell stage, imprinted XCI (iXCI) exclusively silences the paternal X (Xp), and this pattern is maintained in extraembryonic cell types. Epiblast cells, which give rise to the embryo proper, reactivate the Xp (XCR) and undergo a random form of XCI (rXCI) around implantation. Both iXCI and rXCI depend on the long non-coding RNA Xist. The ubiquitin ligase RLIM is required for iXCI in vivo and occupies a central role in current models of rXCI. Here, we demonstrate the existence of Rlim-dependent and Rlim-independent pathways for rXCI in differentiating female ESCs. Upon uncoupling these pathways, we find more efficient Rlim-independent XCI in ESCs cultured under physiological oxygen conditions. Our results revise current models of rXCI and suggest that caution must be taken when comparing XCI studies in ESCs and mice.

Year of Publication
2017
Journal
Cell reports
Volume
21
Issue
13
Number of Pages
3691-3699
Date Published
12/2017
ISSN Number
2211-1247
DOI
10.1016/j.celrep.2017.12.004
Alternate Journal
Cell Rep
PMID
29281819
PMCID
PMC5747310
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