Evidence that random and imprinted Xist expression is controlled by preemptive methylation

The mouse Xist gene is expressed exclusively from the inactive X chromosome and may control the initiation of X inactivation. We show that in somatic tissues the 5′ end of the silent Xist allele on the active X chromosome is fully methylated, while the expressed allele on the inactive X is completel...

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Veröffentlicht in:Cell 1994-04, Vol.77 (1), p.41-51
Hauptverfasser: Norris, Dominic P., Patel, Dipika, Kay, Graham F., Penny, Graeme D., Brockdorff, Neil, Sheardown, Steven A., Rastan, Sohaila
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Sprache:eng
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Zusammenfassung:The mouse Xist gene is expressed exclusively from the inactive X chromosome and may control the initiation of X inactivation. We show that in somatic tissues the 5′ end of the silent Xist allele on the active X chromosome is fully methylated, while the expressed allele on the inactive X is completely unmethylated. In tissues that undergo imprinted paternal Xist expression and imprinted X inactivation, the paternal Xist allele is unmethylated, and the silent maternal allele is fully methylated. In the male germline, a developmentally regulated demethylation of Xist occurs at the onset of meiosis and is retained in mature spermatozoa. This may be the cause of imprinted expression of the paternal Xist allele. A role for methylation in the control of Xist expression is further supported by the finding that in differentiating embryonic stem cells during the initiation of X inactivation, differential methylation of Xist alleles precedes the onset of Xist expression.
ISSN:0092-8674
1097-4172
DOI:10.1016/0092-8674(94)90233-X