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Journal article

The identification and functional annotation of RNA structures conserved in vertebrates

From

University of Copenhagen1

Department of Biotechnology and Biomedicine, Technical University of Denmark2

Regulatory Genomics, Section for Synthetic Biology, Department of Biotechnology and Biomedicine, Technical University of Denmark3

Structured elements of RNA molecules are essential in, e.g., RNA stabilization, localization and protein interaction, and their conservation across species suggests a common functional role. We computationally screened vertebrate genomes for Conserved RNA Structures (CRSs), leveraging structure-based, rather than sequence-based, alignments.

After careful correction for sequence identity and GC content, we predict ~516k human genomic regions containing CRSs. We find that a substantial fraction of human-mouse CRS regions (i) co-localize consistently with binding sites of the same RNA binding proteins (RBPs) or (ii) are transcribed in corresponding tissues.

Additionally, a CaptureSeq experiment revealed expression of many of our CRS regions in human fetal brain, including 662 novel ones. For selected human and mouse candidate pairs, qRT-PCR and in vitro RNA structure probing supported both shared expression and shared structure despite low abundance and low sequence identity.

About 30k CRS regions are located near coding or long non-coding RNA genes or within enhancers. Structured (CRS overlapping) enhancer RNAs and extended 3' ends have significantly increased expression levels over their non-structured counterparts. Our findings of transcribed uncharacterized regulatory regions that contain CRSs support their RNA-mediated functionality.

Language: English
Publisher: Cold Spring Harbor Laboratory Press
Year: 2017
Pages: 1371-1383
ISSN: 15495469 and 10889051
Types: Journal article
DOI: 10.1101/gr.208652.116
ORCIDs: 0000-0002-2359-4927 , 0000-0001-7143-2810 and Workman, Christopher

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