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Literature DB >> 24463464

Topological organization of multichromosomal regions by the long intergenic noncoding RNA Firre.

Ezgi Hacisuleyman¹, Loyal A Goff², Cole Trapnell³, Adam Williams⁴, Jorge Henao-Mejia⁴, Lei Sun⁵, Patrick McClanahan⁶, David G Hendrickson³, Martin Sauvageau³, David R Kelley³, Michael Morse⁷, Jesse Engreitz⁷, Eric S Lander⁷, Mitch Guttman⁸, Harvey F Lodish⁹, Richard Flavell¹⁰, Arjun Raj⁶, John L Rinn¹¹.

Abstract

RNA, including long noncoding RNA (lncRNA), is known to be an abundant and important structural component of the nuclear matrix. However, the molecular identities, functional roles and localization dynamics of lncRNAs that influence nuclear architecture remain poorly understood. Here, we describe one lncRNA, Firre, that interacts with the nuclear-matrix factor hnRNPU through a 156-bp repeating sequence and localizes across an ~5-Mb domain on the X chromosome. We further observed Firre localization across five distinct trans-chromosomal loci, which reside in spatial proximity to the Firre genomic locus on the X chromosome. Both genetic deletion of the Firre locus and knockdown of hnRNPU resulted in loss of colocalization of these trans-chromosomal interacting loci. Thus, our data suggest a model in which lncRNAs such as Firre can interface with and modulate nuclear architecture across chromosomes.

Entities: CellLine Chemical Disease Gene Mutation Species

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Year: 2014 PMID： 24463464 PMCID： PMC3950333 DOI： 10.1038/nsmb.2764

Source DB: PubMed Journal: Nat Struct Mol Biol ISSN： 1545-9985 Impact factor: 15.369

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