Systematic identification and characterization of RNA editing in prostate tumors.

RNA editing modifies the sequence of primary transcripts, potentially resulting in profound effects to RNA structure and protein-coding sequence. Recent analyses of RNA sequence data are beginning to provide insights into the distribution of RNA editing across the entire transcriptome, but there are...

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Main Authors: Fan Mo, Alexander W Wyatt, Yue Sun, Sonal Brahmbhatt, Brian J McConeghy, Chunxiao Wu, Yuzhuo Wang, Martin E Gleave, Stanislav V Volik, Colin C Collins
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2014-01-01
Series:PLoS ONE
Online Access:http://europepmc.org/articles/PMC4103770?pdf=render
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spelling doaj-dba4b5796f804a4991b6973c243dc3522020-11-25T02:33:38ZengPublic Library of Science (PLoS)PLoS ONE1932-62032014-01-0197e10143110.1371/journal.pone.0101431Systematic identification and characterization of RNA editing in prostate tumors.Fan MoAlexander W WyattYue SunSonal BrahmbhattBrian J McConeghyChunxiao WuYuzhuo WangMartin E GleaveStanislav V VolikColin C CollinsRNA editing modifies the sequence of primary transcripts, potentially resulting in profound effects to RNA structure and protein-coding sequence. Recent analyses of RNA sequence data are beginning to provide insights into the distribution of RNA editing across the entire transcriptome, but there are few published matched whole genome and transcriptome sequence datasets, and designing accurate bioinformatics methodology has proven highly challenging. To further characterize the RNA editome, we analyzed 16 paired DNA-RNA sequence libraries from prostate tumor specimens, employing a comprehensive strategy to rescue low coverage sites and minimize false positives. We identified over a hundred thousand putative RNA editing events, a third of which were recurrent in two or more samples, and systematically characterized their type and distribution across the genome. Within genes the majority of events affect non-coding regions such as introns and untranslated regions (UTRs), but 546 genes had RNA editing events predicted to result in deleterious amino acid alterations. Finally, we report a potential association between RNA editing of microRNA binding sites within 3' UTRs and increased transcript expression. These results provide a systematic characterization of the landscape of RNA editing in low coverage sequence data from prostate tumor specimens. We demonstrate further evidence for RNA editing as an important regulatory mechanism and suggest that the RNA editome should be further studied in cancer.http://europepmc.org/articles/PMC4103770?pdf=render
collection DOAJ
language English
format Article
sources DOAJ
author Fan Mo
Alexander W Wyatt
Yue Sun
Sonal Brahmbhatt
Brian J McConeghy
Chunxiao Wu
Yuzhuo Wang
Martin E Gleave
Stanislav V Volik
Colin C Collins
spellingShingle Fan Mo
Alexander W Wyatt
Yue Sun
Sonal Brahmbhatt
Brian J McConeghy
Chunxiao Wu
Yuzhuo Wang
Martin E Gleave
Stanislav V Volik
Colin C Collins
Systematic identification and characterization of RNA editing in prostate tumors.
PLoS ONE
author_facet Fan Mo
Alexander W Wyatt
Yue Sun
Sonal Brahmbhatt
Brian J McConeghy
Chunxiao Wu
Yuzhuo Wang
Martin E Gleave
Stanislav V Volik
Colin C Collins
author_sort Fan Mo
title Systematic identification and characterization of RNA editing in prostate tumors.
title_short Systematic identification and characterization of RNA editing in prostate tumors.
title_full Systematic identification and characterization of RNA editing in prostate tumors.
title_fullStr Systematic identification and characterization of RNA editing in prostate tumors.
title_full_unstemmed Systematic identification and characterization of RNA editing in prostate tumors.
title_sort systematic identification and characterization of rna editing in prostate tumors.
publisher Public Library of Science (PLoS)
series PLoS ONE
issn 1932-6203
publishDate 2014-01-01
description RNA editing modifies the sequence of primary transcripts, potentially resulting in profound effects to RNA structure and protein-coding sequence. Recent analyses of RNA sequence data are beginning to provide insights into the distribution of RNA editing across the entire transcriptome, but there are few published matched whole genome and transcriptome sequence datasets, and designing accurate bioinformatics methodology has proven highly challenging. To further characterize the RNA editome, we analyzed 16 paired DNA-RNA sequence libraries from prostate tumor specimens, employing a comprehensive strategy to rescue low coverage sites and minimize false positives. We identified over a hundred thousand putative RNA editing events, a third of which were recurrent in two or more samples, and systematically characterized their type and distribution across the genome. Within genes the majority of events affect non-coding regions such as introns and untranslated regions (UTRs), but 546 genes had RNA editing events predicted to result in deleterious amino acid alterations. Finally, we report a potential association between RNA editing of microRNA binding sites within 3' UTRs and increased transcript expression. These results provide a systematic characterization of the landscape of RNA editing in low coverage sequence data from prostate tumor specimens. We demonstrate further evidence for RNA editing as an important regulatory mechanism and suggest that the RNA editome should be further studied in cancer.
url http://europepmc.org/articles/PMC4103770?pdf=render
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