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- W2898723770 abstract "Recursive splicing (RS) starts by defining an RS-exon, which is then spliced to the preceding exon, thus creating a recursive 5' splice site (RS-5ss). Previous studies focused on cryptic RS-exons, and now we find that the exon junction complex (EJC) represses RS of hundreds of annotated, mainly constitutive RS-exons. The core EJC factors, and the peripheral factors PNN and RNPS1, maintain RS-exon inclusion by repressing spliceosomal assembly on RS-5ss. The EJC also blocks 5ss located near exon-exon junctions, thus repressing inclusion of cryptic microexons. The prevalence of annotated RS-exons is high in deuterostomes, while the cryptic RS-exons are more prevalent in Drosophila, where EJC appears less capable of repressing RS. Notably, incomplete repression of RS also contributes to physiological alternative splicing of several human RS-exons. Finally, haploinsufficiency of the EJC factor Magoh in mice is associated with skipping of RS-exons in the brain, with relevance to the microcephaly phenotype and human diseases." @default.
- W2898723770 created "2018-11-09" @default.
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- W2898723770 date "2018-11-01" @default.
- W2898723770 modified "2023-10-15" @default.
- W2898723770 title "Exon Junction Complex Shapes the Transcriptome by Repressing Recursive Splicing" @default.
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- W2898723770 doi "https://doi.org/10.1016/j.molcel.2018.09.033" @default.
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