RBFOX2-regulated TEAD1 alternative splicing plays a pivotal role in Hippo-YAP signaling

Author:

Choi Sunkyung1,Lee Hyo Seong1,Cho Namjoon1,Kim Inyoung1ORCID,Cheon Seongmin23,Park Chungoo2,Kim Eun-Mi4,Kim Wantae1,Kim Kee K1ORCID

Affiliation:

1. Department of Biochemistry, College of Natural Sciences, Chungnam National University , Daejeon 34134, Republic of Korea

2. School of Biological Sciences and Technology, Chonnam National University , Gwangju 61186, Republic of Korea

3. Proteomics Core Facility, Biomedical Research Institute, Seoul National University Hospital , Seoul 03080, Republic of Korea

4. Department of Predictive Toxicology, Korea Institute of Toxicology , Daejeon, 34114, Republic of Korea

Abstract

Abstract Alternative pre-mRNA splicing is key to proteome diversity; however, the biological roles of alternative splicing (AS) in signaling pathways remain elusive. Here, we focus on TEA domain transcription factor 1 (TEAD1), a YAP binding factor in the Hippo signaling pathway. Public database analyses showed that expression of YAP-TEAD target genes negatively correlated with the expression of a TEAD1 isoform lacking exon 6 (TEAD1ΔE6) but did not correlate with overall TEAD1 expression. We confirmed that the transcriptional activity and oncogenic properties of the full-length TEAD1 isoform were greater than those of TEAD1ΔE6, with the difference in transcription related to YAP interaction. Furthermore, we showed that RNA-binding Fox-1 homolog 2 (RBFOX2) promoted the inclusion of TEAD1 exon 6 via binding to the conserved GCAUG element in the downstream intron. These results suggest a regulatory mechanism of RBFOX2-mediated TEAD1 AS and provide insight into AS-specific modulation of signaling pathways.

Funder

National Research Foundation of Korea

Korea Environmental Industry and Technology Institute

Publisher

Oxford University Press (OUP)

Subject

Genetics

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