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Authordc.contributor.authorAmaral, Paulo P. 
Authordc.contributor.authorLeonardi, Tommaso 
Authordc.contributor.authorHan, Namshik 
Authordc.contributor.authorVire, Emmanuelle 
Authordc.contributor.authorGascoigne, Dennis K. 
Authordc.contributor.authorArias Carrasco, Raúl 
Authordc.contributor.authorBuscher, Magdalena 
Authordc.contributor.authorPandolfini, Luca 
Authordc.contributor.authorZhang, Anda 
Authordc.contributor.authorPluchino, Stefano 
Authordc.contributor.authorMaracaja Coutinho, Vinicius 
Authordc.contributor.authorNakaya, Helder I. 
Authordc.contributor.authorHemberg, Martin 
Authordc.contributor.authorShiekhattar, Ramin 
Authordc.contributor.authorEnright, Anton J. 
Authordc.contributor.authorKouzarides, Tony 
Admission datedc.date.accessioned2018-07-17T16:28:01Z
Available datedc.date.available2018-07-17T16:28:01Z
Publication datedc.date.issued2018
Cita de ítemdc.identifier.citationGenome Biology (2018) 19:32es_ES
Identifierdc.identifier.other10.1186/s13059-018-1405-5
Identifierdc.identifier.urihttps://repositorio.uchile.cl/handle/2250/149920
Abstractdc.description.abstractBackground: The mammalian genome is transcribed into large numbers of long noncoding RNAs (lncRNAs), but the definition of functional lncRNA groups has proven difficult, partly due to their low sequence conservation and lack of identified shared properties. Here we consider promoter conservation and positional conservation as indicators of functional commonality. Results: We identify 665 conserved lncRNA promoters in mouse and human that are preserved in genomic position relative to orthologous coding genes. These positionally conserved lncRNA genes are primarily associated with developmental transcription factor loci with which they are coexpressed in a tissue-specific manner. Over half of positionally conserved RNAs in this set are linked to chromatin organization structures, overlapping binding sites for the CTCF chromatin organiser and located at chromatin loop anchor points and borders of topologically associating domains (TADs). We define these RNAs as topological anchor point RNAs (tapRNAs). Characterization of these noncoding RNAs and their associated coding genes shows that they are functionally connected: they regulate each other's expression and influence the metastatic phenotype of cancer cells in vitro in a similar fashion. Furthermore, we find that tapRNAs contain conserved sequence domains that are enriched in motifs for zinc finger domain-containing RNA-binding proteins and transcription factors, whose binding sites are found mutated in cancers. Conclusions: This work leverages positional conservation to identify lncRNAs with potential importance in genome organization, development and disease. The evidence that many developmental transcription factors are physically and functionally connected to lncRNAs represents an exciting stepping-stone to further our understanding of genome regulation.es_ES
Patrocinadordc.description.sponsorshipCancer Research UK C6/A18796 C6946/A14492 European Research Council CRIPTON Grant 268569 University of Cambridge FAPESP 2014/50308-4 Wellcome Trust 092096 PAI-CONICYT grant PAI79170021 FONDECYT-CONICYT grant 11161020es_ES
Lenguagedc.language.isoenes_ES
Publisherdc.publisherBIOMED Central Ltd.es_ES
Type of licensedc.rightsAttribution-NonCommercial-NoDerivs 3.0 Chile*
Link to Licensedc.rights.urihttp://creativecommons.org/licenses/by-nc-nd/3.0/cl/*
Keywordsdc.subjectlncRNAses_ES
Keywordsdc.subjectDevelopmentes_ES
Keywordsdc.subjectChromatin architecturees_ES
Keywordsdc.subjectTopologyes_ES
Keywordsdc.subjectZinc fingeres_ES
Keywordsdc.subjectCanceres_ES
Títulodc.titleGenomic positional conservation identifies topological anchor point RNAs linked to developmental locies_ES
Document typedc.typeArtículo de revista
Catalogueruchile.catalogadortjnes_ES
Indexationuchile.indexArtículo de publicación ISIes_ES


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Attribution-NonCommercial-NoDerivs 3.0 Chile
Except where otherwise noted, this item's license is described as Attribution-NonCommercial-NoDerivs 3.0 Chile