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Genetic and epigenetic features direct differential efficiency of Xist-mediated silencing at X-chromosomal and autosomal locations. | LitMetric

AI Article Synopsis

  • Xist RNA is crucial for X chromosome inactivation, but the mechanisms of its selective silencing efficiency across different regions are still unclear.
  • The study involves inducing Xist expression from various locations in mouse cells to analyze its function, revealing that Xist can effectively mimic natural X inactivation from any X chromosome site, while silencing of autosomal genes is less effective.
  • Long interspersed elements aid in silencing genes located far from where Xist is expressed, and genes that resist X inactivation show a particular protein (CTCF) enrichment on X chromosome loci but not on autosomes, indicating unique features of the X chromosome.

Article Abstract

Xist is indispensable for X chromosome inactivation. However, how Xist RNA directs chromosome-wide silencing and why some regions are more efficiently silenced than others remains unknown. Here, we explore the function of Xist by inducing ectopic Xist expression from multiple different X-linked and autosomal loci in mouse aneuploid and female diploid embryonic stem cells in which Xist-mediated silencing does not lead to lethal functional monosomy. We show that ectopic Xist expression faithfully recapitulates endogenous X chromosome inactivation from any location on the X chromosome, whereas long-range silencing of autosomal genes is less efficient. Long interspersed elements facilitate inactivation of genes located far away from the Xist transcription locus, and genes escaping X chromosome inactivation show enrichment of CTCF on X chromosomal but not autosomal loci. Our findings highlight important genomic and epigenetic features acquired during sex chromosome evolution to facilitate an efficient X chromosome inactivation process.Xist RNA is required for X chromosome inactivation but it is not well understood how Xist silences some regions more efficiently than others. Here, the authors induce ectopic Xist expression from multiple different X-linked and autosomal loci in cells to explore Xist function.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC5612955PMC
http://dx.doi.org/10.1038/s41467-017-00528-1DOI Listing

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