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  3. Molecular basis of RNA-binding and autoregulation by the cancer-associated splicing factor RBM39.
 

Molecular basis of RNA-binding and autoregulation by the cancer-associated splicing factor RBM39.

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BORIS DOI
10.48350/186042
Publisher DOI
10.1038/s41467-023-40254-5
PubMed ID
37666821
Description
Pharmacologic depletion of RNA-binding motif 39 (RBM39) using aryl sulfonamides represents a promising anti-cancer therapy but requires high levels of the adaptor protein DCAF15. Consequently, novel approaches to deplete RBM39 in an DCAF15-independent manner are required. Here, we uncover that RBM39 autoregulates via the inclusion of a poison exon into its own pre-mRNA and identify the cis-acting elements that govern this regulation. We also determine the NMR solution structures of RBM39's tandem RNA recognition motifs (RRM1 and RRM2) bound to their respective RNA targets, revealing how RRM1 recognises RNA stem loops whereas RRM2 binds specifically to single-stranded N(G/U)NUUUG. Our results support a model where RRM2 selects the 3'-splice site of a poison exon and the RRM3 and RS domain stabilise the U2 snRNP at the branchpoint. Our work provides molecular insights into RBM39-dependent 3'-splice site selection and constitutes a solid basis to design alternative anti-cancer therapies.
Date of Publication
2023-09-04
Publication Type
Article
Subject(s)
500 Science > 570 Life sciences; biology
500 Science > 540 Chemistry
Language(s)
en
Contributor(s)
Campagne, Sébastien
Jutzi, Daniel
Malard, Florian
Matoga, Maja
Romane, Ksenija
Feldmuller, Miki
Colombo, Martino
Departement für Chemie, Biochemie und Pharmazie (DCBP) Universität Bern
Ruepp, Marc-David
Allain, Frédéric H-T
Additional Credits
Departement für Chemie, Biochemie und Pharmazie (DCBP) Universität Bern
Series
Nature communications
Publisher
Nature Publishing Group
ISSN
2041-1723
Access(Rights)
open.access
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