The target of the DEAH-box NTP triphosphatase Prp43 in Saccharomyces cerevisiae 
spliceosomes is the U2 snRNP-intron interaction.

Fourmann, J. B.; Dybkov, O.; Agafonov, D. E.; Tauchert, M. J.; Urlaub, H.; Ficner, R.; Fabrizio, P.; Lührmann, R.

doi:10.7554/eLife.15564

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The target of the DEAH-box NTP triphosphatase Prp43 in Saccharomyces cerevisiae spliceosomes is the U2 snRNP-intron interaction.

Fourmann, J. B., Dybkov, O., Agafonov, D. E., Tauchert, M. J., Urlaub, H., Ficner, R., et al. (2016). The target of the DEAH-box NTP triphosphatase Prp43 in Saccharomyces cerevisiae spliceosomes is the U2 snRNP-intron interaction. eLife, 5: e15564. doi:10.7554/eLife.15564.

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Creators:
Fourmann, J. B.¹, Author
Dybkov, O.¹, Author
Agafonov, D. E.¹, Author
Tauchert, M. J., Author
Urlaub, H.², Author
Ficner, R., Author
Fabrizio, P.¹, Author
Lührmann, R.¹, Author

Affiliations:
1Department of Cellular Biochemistry, MPI for biophysical chemistry, Max Planck Society, ou_578576
2Research Group of Bioanalytical Mass Spectrometry, MPI for biophysical chemistry, Max Planck Society, ou_578613

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Free keywords: Human; S. cerevisiae; biochemistry; chromosomes; genes; helicases; spliceosome

Abstract: The DEAH-box NTPase Prp43 and its cofactors Ntr1 and Ntr2 form the NTR complex and are required for disassembling intron-lariat spliceosomes (ILS) and defective earlier spliceosomes. However, the Prp43 binding site in the spliceosome and its target(s) are unknown. We show that Prp43 fused to Ntr1's G-patch motif (Prp43_Ntr1GP) is as efficient as the NTR in ILS disassembly, yielding identical dissociation products and recognizing its natural ILS target even in the absence of Ntr1's C-terminal-domain (CTD) and Ntr2. Unlike the NTR, Prp43_Ntr1GP disassembles earlier spliceosomal complexes (A, B, B(act)), indicating that Ntr2/Ntr1-CTD prevents NTR from disrupting properly assembled spliceosomes other than the ILS. The U2 snRNP-intron interaction is disrupted in all complexes by Prp43_Ntr1GP, and in the spliceosome contacts U2 proteins and the pre-mRNA, indicating that the U2 snRNP-intron interaction is Prp43's major target.

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Language(s): eng - English

Dates: Published Online: 2016-04-26

Publication Status: Published online

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Rev. Type: Peer

Identifiers: DOI: 10.7554/eLife.15564

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Title: eLife

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Pages: 17 Volume / Issue: 5 Sequence Number: e15564 Start / End Page: - Identifier: -