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Modulation of pre-mRNA structure by hnRNP proteins regulates alternative splicing of MALT1.


ABSTRACT: Alternative splicing plays key roles for cell type-specific regulation of protein function. It is controlled by cis-regulatory RNA elements that are recognized by RNA binding proteins (RBPs). The MALT1 paracaspase is a key factor of signaling pathways that mediate innate and adaptive immune responses. Alternative splicing of MALT1 is critical for controlling optimal T cell activation. We demonstrate that MALT1 splicing depends on RNA structural elements that sequester the splice sites of the alternatively spliced exon7. The RBPs hnRNP U and hnRNP L bind competitively to stem-loop RNA structures that involve the 5' and 3' splice sites flanking exon7. While hnRNP U stabilizes RNA stem-loop conformations that maintain exon7 skipping, hnRNP L disrupts these RNA elements to facilitate recruitment of the essential splicing factor U2AF2, thereby promoting exon7 inclusion. Our data represent a paradigm for the control of splice site selection by differential RBP binding and modulation of pre-mRNA structure.

SUBMITTER: Jones AN 

PROVIDER: S-EPMC9348792 | biostudies-literature | 2022 Aug

REPOSITORIES: biostudies-literature

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Modulation of pre-mRNA structure by hnRNP proteins regulates alternative splicing of <i>MALT1</i>.

Jones Alisha N AN   Graß Carina C   Meininger Isabel I   Geerlof Arie A   Klostermann Melina M   Zarnack Kathi K   Krappmann Daniel D   Sattler Michael M  

Science advances 20220803 31


Alternative splicing plays key roles for cell type-specific regulation of protein function. It is controlled by cis-regulatory RNA elements that are recognized by RNA binding proteins (RBPs). The MALT1 paracaspase is a key factor of signaling pathways that mediate innate and adaptive immune responses. Alternative splicing of <i>MALT1</i> is critical for controlling optimal T cell activation. We demonstrate that <i>MALT1</i> splicing depends on RNA structural elements that sequester the splice si  ...[more]

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