RBFOX2 Is an Important Regulator of Mesenchymal Tissue-Specific Splicing in both Normal and Cancer Tissues

J. P. Venables(Université de Sherbrooke), Jean-Philippe Brosseau(Université de Sherbrooke), Gilles Gadéa(Centre de Recherche en Biologie cellulaire de Montpellier), Roscoe Klinck(Université de Sherbrooke), Panagiotis Prinos(Université de Sherbrooke), Jean‐François Beaulieu(Université de Sherbrooke), Elvy Lapointe(Université de Sherbrooke), Mathieu Durand(Université de Sherbrooke), Philippe Thibault(Université de Sherbrooke), Karine Tremblay(Université de Sherbrooke), François Rousset(Centre National de la Recherche Scientifique), Jamal Tazi(Institut de Génétique Moléculaire de Montpellier), Sherif Abou Elela(Université de Sherbrooke), Benoı̂t Chabot(Université de Sherbrooke)
Molecular and Cellular Biology
November 13, 2012
Cited by 156Open Access
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Abstract

Alternative splicing provides a critical and flexible layer of regulation intervening in many biological processes to regulate the diversity of proteins and impact cell phenotype. To identify alternative splicing differences that distinguish epithelial from mesenchymal tissues, we have investigated hundreds of cassette exons using a high-throughput reverse transcription-PCR (RT-PCR) platform. Extensive changes in splicing were noted between epithelial and mesenchymal tissues in both human colon and ovarian tissues, with many changes from mostly one splice variant to predominantly the other. Remarkably, many of the splicing differences that distinguish normal mesenchymal from normal epithelial tissues matched those that differentiate normal ovarian tissues from ovarian cancer. Furthermore, because splicing profiling could classify cancer cell lines according to their epithelial/mesenchymal characteristics, we used these cancer cell lines to identify regulators for these specific splicing signatures. By knocking down 78 potential splicing factors in five cell lines, we provide an extensive view of the complex regulatory landscape associated with the epithelial and mesenchymal states, thus revealing that RBFOX2 is an important driver of mesenchymal tissue-specific splicing.


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