An Xist-activating antisense RNA required for X-chromosome inactivation

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Mrinal K. Sarkar
Srimonta Gayen
Surinder Kumar
Emily Maclary
Emily Buttigieg
Michael Hinten
Archana Kumari
Clair Harris
Takashi Sado
Sundeep Kalantry
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[1] University of Michigan Medical School,Department of Human Genetics
[2] Graduate School of Agriculture,Department of Advanced Bioscience
[3] Kinki University,undefined
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The transcriptional imbalance due to the difference in the number of X chromosomes between male and female mammals is remedied through X-chromosome inactivation, the epigenetic transcriptional silencing of one of the two X chromosomes in females. The X-linked Xist long non-coding RNA functions as an X inactivation master regulator; Xist is selectively upregulated from the prospective inactive X chromosome and is required in cis for X inactivation. Here we discover an Xist antisense long non-coding RNA, XistAR (XistActivating RNA), which is encoded within exon 1 of the mouse Xist gene and is transcribed only from the inactive X chromosome. Selective truncation of XistAR, while sparing the overlapping Xist RNA, leads to a deficiency in Xist RNA expression in cis during the initiation of X inactivation. Thus, the Xist gene carries within its coding sequence an antisense RNA that drives Xist expression.
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