AI Article Synopsis

  • The inactive X-chromosome (Xi) in mammals has a unique 3D structure that differs from other chromosomes, organized into megadomains and superloops.
  • Noncoding loci Dxz4 and Firre influence these structures but their exact roles are uncertain; disrupting them doesn't affect Xi gene silencing or escape from inactivation.
  • The study concludes that both Dxz4 and megadomains are not necessary for Xi silencing or for the expression of genes that escape X-inactivation.

Article Abstract

The mammalian inactive X-chromosome (Xi) is structurally distinct from all other chromosomes and serves as a model for how the 3D genome is organized. The Xi shows weakened topologically associated domains and is instead organized into megadomains and superloops directed by the noncoding loci, Dxz4 and Firre. Their functional significance is presently unclear, though one study suggests that they permit Xi genes to escape silencing. Here, we find that megadomains do not precede Xist expression or Xi gene silencing. Deleting Dxz4 disrupts the sharp megadomain border, whereas deleting Firre weakens intra-megadomain interactions. However, deleting Dxz4 and/or Firre has no impact on Xi silencing and gene escape. Nor does it affect Xi nuclear localization, stability, or H3K27 methylation. Additionally, ectopic integration of Dxz4 and Xist is not sufficient to form megadomains on autosomes. We conclude that Dxz4 and megadomains are dispensable for Xi silencing and escape from X-inactivation.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC6258728PMC
http://dx.doi.org/10.1038/s41467-018-07446-wDOI Listing

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