Literature DB >> 17210931

Widespread mRNA polyadenylation events in introns indicate dynamic interplay between polyadenylation and splicing.

Bin Tian1, Zhenhua Pan, Ju Youn Lee.   

Abstract

mRNA polyadenylation and pre-mRNA splicing are two essential steps for the maturation of most human mRNAs. Studies have shown that some genes generate mRNA variants involving both alternative polyadenylation and alternative splicing. Polyadenylation in introns can lead to conversion of an internal exon to a 3' terminal exon, which is termed composite terminal exon, or usage of a 3' terminal exon that is otherwise skipped, which is termed skipped terminal exon. Using cDNA/EST and genome sequences, we identified polyadenylation sites in introns for all currently known human genes. We found that approximately 20% human genes have at least one intronic polyadenylation event that can potentially lead to mRNA variants, most of which encode different protein products. The conservation of human intronic poly(A) sites in mouse and rat genomes is lower than that of poly(A) sites in 3'-most exons. Quantitative analysis of a number of mRNA variants generated by intronic poly(A) sites suggests that the intronic polyadenylation activity can vary under different cellular conditions for most genes. Furthermore, we found that weak 5' splice site and large intron size are the determining factors controlling the usage of composite terminal exon poly(A) sites, whereas skipped terminal exon poly(A) sites tend to be associated with strong polyadenylation signals. Thus, our data indicate that dynamic interplay between polyadenylation and splicing leads to widespread polyadenylation in introns and contributes to the complexity of transcriptome in the cell.

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Year:  2007        PMID: 17210931      PMCID: PMC1781347          DOI: 10.1101/gr.5532707

Source DB:  PubMed          Journal:  Genome Res        ISSN: 1088-9051            Impact factor:   9.043


  58 in total

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4.  Prediction of mRNA polyadenylation sites by support vector machine.

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5.  Direct interactions between subunits of CPSF and the U2 snRNP contribute to the coupling of pre-mRNA 3' end processing and splicing.

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Journal:  Mol Cell       Date:  2006-07-21       Impact factor: 17.970

6.  Local similarity in RNA secondary structures.

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7.  General and specific functions of exonic splicing silencers in splicing control.

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8.  An interaction between U2AF 65 and CF I(m) links the splicing and 3' end processing machineries.

Authors:  Stefania Millevoi; Clarisse Loulergue; Sabine Dettwiler; Sarah Zeïneb Karaa; Walter Keller; Michael Antoniou; Stéphan Vagner
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9.  An intronic polyadenylation site in human and mouse CstF-77 genes suggests an evolutionarily conserved regulatory mechanism.

Authors:  Zhenhua Pan; Haibo Zhang; Lisa K Hague; Ju Youn Lee; Carol S Lutz; Bin Tian
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10.  A third approach to gene prediction suggests thousands of additional human transcribed regions.

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  114 in total

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2.  Alternative splicing and polyadenylation contribute to the generation of hERG1 C-terminal isoforms.

Authors:  Qiuming Gong; Matthew R Stump; A Russell Dunn; Vivianne Deng; Zhengfeng Zhou
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Review 5.  The Schistosoma mansoni transcriptome: an update.

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Review 7.  Alternative cleavage and polyadenylation: extent, regulation and function.

Authors:  Ran Elkon; Alejandro P Ugalde; Reuven Agami
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Review 8.  Signals for pre-mRNA cleavage and polyadenylation.

Authors:  Bin Tian; Joel H Graber
Journal:  Wiley Interdiscip Rev RNA       Date:  2011-10-19       Impact factor: 9.957

9.  Codon usage biases co-evolve with transcription termination machinery to suppress premature cleavage and polyadenylation.

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Journal:  Elife       Date:  2018-03-16       Impact factor: 8.140

10.  mountainClimber Identifies Alternative Transcription Start and Polyadenylation Sites in RNA-Seq.

Authors:  Ashley A Cass; Xinshu Xiao
Journal:  Cell Syst       Date:  2019-09-18       Impact factor: 10.304

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