TY - JOUR T1 - Trans- and cis-acting effects of the lncRNA <em>Firre</em> on epigenetic and structural features of the inactive X chromosome JF - bioRxiv DO - 10.1101/687236 SP - 687236 AU - He Fang AU - Giancarlo Bonora AU - Jordan P. Lewandowski AU - Jitendra Thakur AU - Galina N. Filippova AU - Steven Henikoff AU - Jay Shendure AU - Zhijun Duan AU - John L. Rinn AU - Xinxian Deng AU - William S. Noble AU - Christine M. Disteche Y1 - 2019/01/01 UR - http://biorxiv.org/content/early/2019/06/30/687236.abstract N2 - Firre encodes a lncRNA involved in nuclear organization in mammals. Here we find that Firre RNA is transcribed from the active X chromosome (Xa) and exerts trans-acting effects on the inactive X chromosome (Xi). Allelic deletion of Firre on the Xa in a mouse hybrid fibroblast cell line results in a dramatic loss of the histone modification H3K27me3 and of components of the PRC2 complex on the Xi as well as the disruption of the perinucleolar location of the Xi. These features are measurably rescued by ectopic expression of a mouse or human Firre/FIRRE cDNA transgene, strongly supporting a conserved trans-acting role of the Firre transcript in maintaining the Xi heterochromatin environment. Surprisingly, CTCF occupancy is decreased on the Xi upon loss of Firre RNA, but is partially recovered by ectopic transgene expression, suggesting a functional link between Firre RNA and CTCF in maintenance of epigenetic features and/or location of the Xi. Loss of Firre RNA results in dysregulation of genes implicated in cell division and development, but not in reactivation of genes on the Xi, which retains its bipartite structure despite some changes in chromatin contact distribution. Allelic deletion or inversion of Firre on the Xi causes localized redistribution of chromatin contacts, apparently dependent on the orientation of CTCF binding sites clustered at the locus. Thus, the Firre locus and its RNA have roles in the maintenance of epigenetic features and structure of the Xi. ER -