Mammalian PRP4 kinase copurifies and interacts with components of both the U5 
snRNP and the N-CoR deacetylase complexes

Dellaire, G.; Makarov, E. M.; Cowger, J. J. M.; Longman, D.; Sutherland, H. G. E.; Luehrmann, R.; Torchia, J.; Bickmore, W. A.

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Mammalian PRP4 kinase copurifies and interacts with components of both the U5 snRNP and the N-CoR deacetylase complexes

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Makarov, E. M.
Department of Cellular Biochemistry, MPI for biophysical chemistry, Max Planck Society;

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Luehrmann, R.
Department of Cellular Biochemistry, MPI for biophysical chemistry, Max Planck Society;

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Dellaire, G., Makarov, E. M., Cowger, J. J. M., Longman, D., Sutherland, H. G. E., Luehrmann, R., et al. (2002). Mammalian PRP4 kinase copurifies and interacts with components of both the U5 snRNP and the N-CoR deacetylase complexes. Molecular and Cellular Biology, 22(14), 5141-5156. Retrieved from http://mcb.asm.org/cgi/reprint/22/14/5141.

Zitierlink: https://hdl.handle.net/11858/00-001M-0000-0010-94EC-D

Zusammenfassung

A growing body of evidence supports the coordination of pre- mRNA processing and transcriptional regulation. We demonstrate here that mammalian PRP4 kinase (PRP4K) is associated with complexes involved in both of these processes. PRP4K is implicated in pre-mRNA splicing as the homologue of the Schizosaccharomyces pombe pre-mRNA splicing kinase Prp4p, and it is enriched in SC35-containing nuclear splicing speckles. RNA interference of Caenorhabditis elegans PRP4K indicates that it is essential in metazoans. In support of a role for PRP4K in pre-mRNA splicing, we identified PRP6, SWAP, and pinin as interacting proteins and demonstrated that PRP4K is a U5 snRNP- associated kinase. In addition, BRG1 and N-CoR, components of nuclear hormone coactivator and corepressor complexes, also interact with PRP4K. PRP4K coimmunoprecipitates with N-CoR, BRG1, pinin, and PRP6, and we present data suggesting that PRP6 and BRG1 are substrates of this kinase. Lastly, PRP4K, BRG1, and PRP6 can be purified as components of the N-CoR-2 complex, and affinity-purified PRP4K/N-CoR complexes exhibit deacetylase activity. We suggest that PRP4K is an essential kinase that, in association with the both U5 snRNP and N-CoR deacetylase complexes, demonstrates a possible coordination of pre-mRNA splicing with chromatin remodeling events involved in transcriptional regulation.