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Arabidopsis <scp>PTB</scp> 1 and <scp>PTB</scp> 2 proteins negatively regulate splicing of a mini‐exon splicing reporter and affect alternative splicing of endogenous genes differentially

Authors :
Michele Liney
Dominika Lewandowska
Sean Chapman
Paul Shaw
John W. S. Brown
James W. McNicol
John L. Fuller
Diane Davidson
Craig G. Simpson
Source :
New Phytologist. 203:424-436
Publication Year :
2014
Publisher :
Wiley, 2014.

Abstract

Summary This paper examines the function of Arabidopsis thaliana AtPTB1 and AtPTB2 as plant splicing factors. The effect on splicing of overexpression of AtPTB1 and AtPTB2 was analysed in an in vivo protoplast transient expression system with a novel mini-exon splicing reporter. A range of mutations in pyrimidine-rich sequences were compared with and without AtPTB and NpU2AF65 overexpression. Splicing analyses of constructs in protoplasts and RNA from overexpression lines used high-resolution reverse transcription polymerase chain reaction (RT-PCR). AtPTB1 and AtPTB2 reduced inclusion/splicing of the potato invertase mini-exon splicing reporter, indicating that these proteins can repress plant intron splicing. Mutation of the polypyrimidine tract and closely associated Cytosine and Uracil-rich (CU-rich) sequences, upstream of the mini-exon, altered repression by AtPTB1 and AtPTB2. Coexpression of a plant orthologue of U2AF65 alleviated the splicing repression of AtPTB1. Mutation of a second CU-rich upstream of the mini-exon 3′ splice site led to a decline in mini-exon splicing, indicating the presence of a splicing enhancer sequence. Finally, RT-PCR of AtPTB overexpression lines with c. 90 known alternative splicing (AS) events showed that AtPTBs significantly altered AS of over half the events. AtPTB1 and AtPTB2 are splicing factors that influence alternative splicing. This occurs in the potato invertase mini-exon via the polypyrimidine tract and associated pyrimidine-rich sequence.

Details

ISSN :
14698137 and 0028646X
Volume :
203
Database :
OpenAIRE
Journal :
New Phytologist
Accession number :
edsair.doi.dedup.....43da1dc9bdadc63e4e7830541d4daf65
Full Text :
https://doi.org/10.1111/nph.12821