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Literature DB >> 25087874

Rbfox2-coordinated alternative splicing of Mef2d and Rock2 controls myoblast fusion during myogenesis.

Ravi K Singh¹, Zheng Xia^2,3, Christopher S Bland⁴, Auinash Kalsotra¹, Marissa A Scavuzzo¹, Tomaz Curk⁵, Jernej Ule⁶, Wei Li^2,3, Thomas A Cooper^1,2,7.

Abstract

Alternative splicing plays important regulatory roles during periods of physiological change. During development, a large number of genes coordinately express protein isoform transitions regulated by alternative splicing; however, the mechanisms that coordinate splicing and the functional integration of the resultant tissue-specific protein isoforms are typically unknown. Here we show that the conserved Rbfox2 RNA binding protein regulates 30% of the splicing transitions observed during myogenesis and is required for the specific step of myoblast fusion. Integration of Rbfox2-dependent splicing outcomes from RNA-seq with Rbfox2 iCLIP data identified Mef2d and Rock2 as Rbfox2 splicing targets. Restored activities of Mef2d and Rock2 rescued myoblast fusion in Rbfox2-depleted cultures, demonstrating functional cooperation of protein isoforms generated by coordinated alterative splicing. The results demonstrate that coordinated alternative splicing by a single RNA binding protein modulates transcription (Mef2d) and cell signaling (Rock2) programs to drive tissue-specific functions (cell fusion) to promote a developmental transition.

Entities: Chemical

Mesh：

Substances：

Year: 2014 PMID： 25087874 PMCID： PMC4142074 DOI： 10.1016/j.molcel.2014.06.035

Source DB: PubMed Journal: Mol Cell ISSN： 1097-2765 Impact factor: 17.970

48 in total

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58 in total

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