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A comprehensive analysis of 3' end sequencing data sets reveals novel polyadenylation signals and the repressive role of heterogeneous ribonucleoprotein C on cleavage and polyadenylation

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2016

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Schmidt, Ralf
Gruber, Andreas R.
Martin, Georges
Ghosh, Souvik
Belmadani, Manuel
Keller, Walter
Zavolan, Mihaela

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Genome Research. Cold Spring Harbor Laboratory Press. 2016, 26(8), pp. 1145-1159. ISSN 1054-9803. eISSN 1549-5469. Available under: doi: 10.1101/gr.202432.115

Zusammenfassung

Alternative polyadenylation (APA) is a general mechanism of transcript diversification in mammals, which has been recently linked to proliferative states and cancer. Different 3' untranslated region (3' UTR) isoforms interact with different RNA-binding proteins (RBPs), which modify the stability, translation, and subcellular localization of the corresponding transcripts. Although the heterogeneity of pre-mRNA 3' end processing has been established with high-throughput approaches, the mechanisms that underlie systematic changes in 3' UTR lengths remain to be characterized. Through a uniform analysis of a large number of 3' end sequencing data sets, we have uncovered 18 signals, six of which are novel, whose positioning with respect to pre-mRNA cleavage sites indicates a role in pre-mRNA 3' end processing in both mouse and human. With 3' end sequencing we have demonstrated that the heterogeneous ribonucleoprotein C (HNRNPC), which binds the poly(U) motif whose frequency also peaks in the vicinity of polyadenylation (poly(A)) sites, has a genome-wide effect on poly(A) site usage. HNRNPC-regulated 3' UTRs are enriched in ELAV-like RBP 1 (ELAVL1) binding sites and include those of the CD47 gene, which participate in the recently discovered mechanism of 3' UTR-dependent protein localization (UDPL). Our study thus establishes an up-to-date, high-confidence catalog of 3' end processing sites and poly(A) signals, and it uncovers an important role of HNRNPC in regulating 3' end processing. It further suggests that U-rich elements mediate interactions with multiple RBPs that regulate different stages in a transcript's life cycle.

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570 Biowissenschaften, Biologie

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ISO 690GRUBER, Andreas J., Ralf SCHMIDT, Andreas R. GRUBER, Georges MARTIN, Souvik GHOSH, Manuel BELMADANI, Walter KELLER, Mihaela ZAVOLAN, 2016. A comprehensive analysis of 3' end sequencing data sets reveals novel polyadenylation signals and the repressive role of heterogeneous ribonucleoprotein C on cleavage and polyadenylation. In: Genome Research. Cold Spring Harbor Laboratory Press. 2016, 26(8), pp. 1145-1159. ISSN 1054-9803. eISSN 1549-5469. Available under: doi: 10.1101/gr.202432.115
BibTex
@article{Gruber2016compr-50940,
  year={2016},
  doi={10.1101/gr.202432.115},
  title={A comprehensive analysis of 3' end sequencing data sets reveals novel polyadenylation signals and the repressive role of heterogeneous ribonucleoprotein C on cleavage and polyadenylation},
  number={8},
  volume={26},
  issn={1054-9803},
  journal={Genome Research},
  pages={1145--1159},
  author={Gruber, Andreas J. and Schmidt, Ralf and Gruber, Andreas R. and Martin, Georges and Ghosh, Souvik and Belmadani, Manuel and Keller, Walter and Zavolan, Mihaela}
}
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