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AKAP95 regulates splicing through scaffolding RNAs and RNA processing factors

Hu, J.
Khodadadi-Jamayran, A.
Mao, M.
Shah, K.
Yang, Z.
Nasim, Md. Talat
Wang, Z.
Jiang, H.
Publication Date
2016-11
End of Embargo
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Rights
© 2016 Hu J et al. This work is licensed under a CC BY license (Creative Commons Attribution 4.0 International License)
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openAccess
Accepted for publication
2016-09-22
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Abstract
Alternative splicing of pre-mRNAs significantly contributes to the complexity of gene expression in higher organisms, but the regulation of the splice site selection remains incompletely understood. We have previously demonstrated that a chromatin-associated protein, AKAP95 (AKAP8), has a remarkable activity in enhancing chromatin transcription. In this study, we have shown that AKAP95 physically interacts with many factors involved in transcription and RNA processing, and functionally regulates pre-mRNA splicing. AKAP95 directly promotes splicing in vitro and the inclusion of a specific exon of an endogenous gene FAM126A. The N-terminal YG-rich domain of AKAP95 is important for its binding to RNA processing factors including selective groups of hnRNP proteins, and its zinc finger domains are critical for pre-mRNA binding. Genome-wide binding assays revealed that AKAP95 bound preferentially to proximal intronic regions on a large number of pre-mRNAs in human transcriptome, and AKAP95 depletion predominantly resulted in reduced inclusion of many exons. AKAP95 also selectively coordinates with hnRNP H/F and U proteins in regulating alternative splicing events. We have further shown that AKAP95 directly interacts with itself. Taken together, our results establish AKAP95 as a novel and mostly positive regulator of premRNA splicing and a possible integrator of transcription and splicing regulation, and support a model that AKAP95 facilitates the splice site communication by looping out introns through both RNA-binding and protein-protein interaction.
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Citation
Hu J, Khodadadi-Jamayran A, Mao M et al (2016) AKAP95 regulates splicing through scaffolding RNAs and RNA processing factors. Nature Communications. 7: Article 13347.
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