Differential alternative splicing activity of isoforms of polypyrimidine tract binding protein (PTB)

MATTHEW C. WOLLERTON; CLARE GOODING; FIONA ROBINSON; EMMA C. BROWN; RICHARD J. JACKSON; CHRISTOPHER W.J. SMITH

doi:10.1017/S1355838201010214

Abstract

Polypyrimidine tract binding protein (PTB) is an RNA-binding protein that regulates splicing by repressing specific splicing events. It also has roles in 3′-end processing, internal initiation of translation, and RNA localization. PTB exists in three alternatively spliced isoforms, PTB1, PTB2, and PTB4, which differ by the insertion of 19 or 26 amino acids, respectively, between the second and third RNA recognition motif domains. Here we show that the PTB isoforms have distinct activities upon α-tropomyosin (TM) alternative splicing. PTB1 reduced the repression of TM exon 3 in transfected smooth muscle cells, whereas PTB4 enhanced TM exon 3 skipping in vivo and in vitro. PTB2 had an intermediate effect. The PTB4 > PTB2 > PTB1 repressive hierarchy was observed in all in vivo and in vitro assays with TM, but the isoforms were equally active in inducing skipping of α-actinin exons and showed the opposite hierarchy of activity when tested for activation of IRES-driven translation. These findings establish that the ratio of PTB isoforms could form part of a cellular code that in turn controls the splicing of various other pre-mRNAs.

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Differential alternative splicing activity of isoforms of polypyrimidine tract binding protein (PTB)

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Differential alternative splicing activity of isoforms of polypyrimidine tract binding protein (PTB)

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