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Post-transcriptional exon shuffling events in humans can be evolutionarily conserved and abundant

Lookup NU author(s): Haya AL-Balool, Dr Mark Wade, Dr Jonathan Coxhead, Professor Julie Irving, Professor David Elliott, Dr Andrew Hall, Dr Mauro Santibanez Koref, Dr Michael Jackson

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Abstract

In silico analyses have established that transcripts from some genes can be processed into RNAs with rearranged exon order relative to genomic structure (post-transcriptional exon shuffling, or PTES). Although known to contribute to transcriptome diversity in some species, to date the structure, distribution, abundance, and functional significance of human PTES transcripts remains largely unknown. Here, using high-throughput transcriptome sequencing, we identify 205 putative human PTES products from 176 genes. We validate 72 out of 112 products analyzed using RT-PCR, and identify additional PTES products structurally related to 61% of validated targets. Sequencing of these additional products reveals GT-AG dinucleotides at >95% of the splice junctions, confirming that they are processed by the spliceosome. We show that most PTES transcripts are expressed in a wide variety of human tissues, that they can be polyadenylated, and that some are conserved in mouse. We also show that they can extend into 5' and 3' UTRs, consistent with formation via trans-splicing of independent pre-mRNA molecules. Finally, we use real-time PCR to compare the abundance of PTES exon junctions relative to canonical exon junctions within the transcripts from seven genes. PTES exon junctions are present at <0.01% to >90% of the levels of canonical junctions, with transcripts from MAN1A2, PHC3, TLE4, and CDK13 exhibiting the highest levels. This is the first systematic experimental analysis of PTES in human, and it suggests both that the phenomenon is much more widespread than previously thought and that some PTES transcripts could be functional.


Publication metadata

Author(s): Al-Balool HH, Weber D, Liu Y, Wade M, Guleria K, Nam PL, Clayton J, Rowe W, Coxhead J, Irving J, Elliott DJ, Hall AG, Santibanez-Koref M, Jackson MS

Publication type: Article

Publication status: Published

Journal: Genome Research

Year: 2011

Volume: 21

Issue: 11

Pages: 1788-1799

Print publication date: 23/09/2011

ISSN (print): 1088-9051

ISSN (electronic): 1549-5469

Publisher: Cold Spring Harbor Laboratory Press

URL: http://dx.doi.org/10.1101/gr.116442.110

DOI: 10.1101/gr.116442.110


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Funding

Funder referenceFunder name
Government of Kuwait
Newcastle Healthcare Charity
ORSAS
Tyne-side Leukaemia Research Association
BB/D013917/1BBSRC
WT080368MAWellcome Trust

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