Promiscuity of enhancer, coding and non-coding transcription functions in ultraconserved elements

Promiscuity of enhancer, coding and non-coding transcription functions in ultraconserved elements

<p>Abstract</p> <p>Background</p> <p>Ultraconserved elements (UCEs) are highly constrained elements of mammalian genomes, whose functional role has not been completely elucidated yet. Previous studies have shown that some of them act as enhancers in mouse, while some ot...

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Main Authors: Sanges Remo, Petrera Francesca, Gennarino Vincenzo A, Licastro Danilo, Banfi Sandro, Stupka Elia
Format: Article
Language:English
Published: BMC 2010-03-01
Series:BMC Genomics
Online Access:http://www.biomedcentral.com/1471-2164/11/151
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spelling doaj-2eeda2e6051e40ae85ff4f25f6d3c07f2020-11-25T00:33:28ZengBMCBMC Genomics1471-21642010-03-0111115110.1186/1471-2164-11-151Promiscuity of enhancer, coding and non-coding transcription functions in ultraconserved elementsSanges RemoPetrera FrancescaGennarino Vincenzo ALicastro DaniloBanfi SandroStupka Elia<p>Abstract</p> <p>Background</p> <p>Ultraconserved elements (UCEs) are highly constrained elements of mammalian genomes, whose functional role has not been completely elucidated yet. Previous studies have shown that some of them act as enhancers in mouse, while some others are expressed in both normal and cancer-derived human tissues. Only one UCE element so far was shown to present these two functions concomitantly, as had been observed in other isolated instances of single, non ultraconserved enhancer elements.</p> <p>Results</p> <p>We used a custom microarray to assess the levels of UCE transcription during mouse development and integrated these data with published microarray and next-generation sequencing datasets as well as with newly produced PCR validation experiments. We show that a large fraction of non-exonic UCEs is transcribed across all developmental stages examined from only one DNA strand. Although the nature of these transcripts remains a mistery, our meta-analysis of RNA-Seq datasets indicates that they are unlikely to be short RNAs and that some of them might encode nuclear transcripts. In the majority of cases this function overlaps with the already established enhancer function of these elements during mouse development. Utilizing several next-generation sequencing datasets, we were further able to show that the level of expression observed in non-exonic UCEs is significantly higher than in random regions of the genome and that this is also seen in other regions which act as enhancers.</p> <p>Conclusion</p> <p>Our data shows that the concurrent presence of enhancer and transcript function in non-exonic UCE elements is more widespread than previously shown. Moreover through our own experiments as well as the use of next-generation sequencing datasets, we were able to show that the RNAs encoded by non-exonic UCEs are likely to be long RNAs transcribed from only one DNA strand.</p> http://www.biomedcentral.com/1471-2164/11/151
collection DOAJ
language English
format Article
sources DOAJ
author Sanges Remo
Petrera Francesca
Gennarino Vincenzo A
Licastro Danilo
Banfi Sandro
Stupka Elia
spellingShingle Sanges Remo
Petrera Francesca
Gennarino Vincenzo A
Licastro Danilo
Banfi Sandro
Stupka Elia
Promiscuity of enhancer, coding and non-coding transcription functions in ultraconserved elements
BMC Genomics
author_facet Sanges Remo
Petrera Francesca
Gennarino Vincenzo A
Licastro Danilo
Banfi Sandro
Stupka Elia
author_sort Sanges Remo
title Promiscuity of enhancer, coding and non-coding transcription functions in ultraconserved elements
title_short Promiscuity of enhancer, coding and non-coding transcription functions in ultraconserved elements
title_full Promiscuity of enhancer, coding and non-coding transcription functions in ultraconserved elements
title_fullStr Promiscuity of enhancer, coding and non-coding transcription functions in ultraconserved elements
title_full_unstemmed Promiscuity of enhancer, coding and non-coding transcription functions in ultraconserved elements
title_sort promiscuity of enhancer, coding and non-coding transcription functions in ultraconserved elements
publisher BMC
series BMC Genomics
issn 1471-2164
publishDate 2010-03-01
description <p>Abstract</p> <p>Background</p> <p>Ultraconserved elements (UCEs) are highly constrained elements of mammalian genomes, whose functional role has not been completely elucidated yet. Previous studies have shown that some of them act as enhancers in mouse, while some others are expressed in both normal and cancer-derived human tissues. Only one UCE element so far was shown to present these two functions concomitantly, as had been observed in other isolated instances of single, non ultraconserved enhancer elements.</p> <p>Results</p> <p>We used a custom microarray to assess the levels of UCE transcription during mouse development and integrated these data with published microarray and next-generation sequencing datasets as well as with newly produced PCR validation experiments. We show that a large fraction of non-exonic UCEs is transcribed across all developmental stages examined from only one DNA strand. Although the nature of these transcripts remains a mistery, our meta-analysis of RNA-Seq datasets indicates that they are unlikely to be short RNAs and that some of them might encode nuclear transcripts. In the majority of cases this function overlaps with the already established enhancer function of these elements during mouse development. Utilizing several next-generation sequencing datasets, we were further able to show that the level of expression observed in non-exonic UCEs is significantly higher than in random regions of the genome and that this is also seen in other regions which act as enhancers.</p> <p>Conclusion</p> <p>Our data shows that the concurrent presence of enhancer and transcript function in non-exonic UCE elements is more widespread than previously shown. Moreover through our own experiments as well as the use of next-generation sequencing datasets, we were able to show that the RNAs encoded by non-exonic UCEs are likely to be long RNAs transcribed from only one DNA strand.</p>
url http://www.biomedcentral.com/1471-2164/11/151
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