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Literature DB >> 25825154

DEAD-box helicase DDX27 regulates 3' end formation of ribosomal 47S RNA and stably associates with the PeBoW-complex.

Markus Kellner¹, Michaela Rohrmoser¹, Ignasi Forné², Kirsten Voss¹, Kaspar Burger¹, Bastian Mühl¹, Anita Gruber-Eber¹, Elisabeth Kremmer³, Axel Imhof², Dirk Eick⁴.

Abstract

PeBoW, a trimeric complex consisting of pescadillo (Pes1), block of proliferation (Bop1), and the WD repeat protein 12 (WDR12), is essential for processing and maturation of mammalian 5.8S and 28S ribosomal RNAs. Applying a mass spectrometric analysis, we identified the DEAD-box helicase DDX27 as stably associated factor of the PeBoW-complex. DDX27 interacts with the PeBoW-complex via an evolutionary conserved F×F motif in the N-terminal domain and is recruited to the nucleolus via its basic C-terminal domain. This recruitment is RNA-dependent and occurs independently of the PeBoW-complex. Interestingly, knockdown of DDX27, but not of Pes1, induces the accumulation of an extended form of the primary 47S rRNA. We conclude that DDX27 can interact specifically with the Pes1 and Bop1 but fulfils critical function(s) for proper 3' end formation of 47S rRNA independently of the PeBoW-complex.

Entities: Gene Species

Keywords: DEAD-box helicase; F×F motif; Nucleolus; PeBoW-complex; rRNA processing

Mesh：

Substances：

Year: 2015 PMID： 25825154 DOI： 10.1016/j.yexcr.2015.03.017

Source DB: PubMed Journal: Exp Cell Res ISSN： 0014-4827 Impact factor: 3.905

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Cited

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DEAD-box helicase DDX27 regulates 3' end formation of ribosomal 47S RNA and stably associates with the PeBoW-complex.

1. Nol12 is a multifunctional RNA binding protein at the nexus of RNA and DNA metabolism.

Review 2. DEAD-ly Affairs: The Roles of DEAD-Box Proteins on HIV-1 Viral RNA Metabolism.

3. Characterisation of a nucleo-adhesome.

4. Concerted removal of the Erb1-Ytm1 complex in ribosome biogenesis relies on an elaborate interface.

5. RNA helicase, DDX27 regulates skeletal muscle growth and regeneration by modulation of translational processes.

6. MIR sequences recruit zinc finger protein ZNF768 to expressed genes.

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