Literature DB >> 16738661

Hrr25-dependent phosphorylation state regulates organization of the pre-40S subunit.

Thorsten Schäfer1, Bohumil Maco, Elisabeth Petfalski, David Tollervey, Bettina Böttcher, Ueli Aebi, Ed Hurt.   

Abstract

The formation of eukaryotic ribosomes is a multistep process that takes place successively in the nucleolar, nucleoplasmic and cytoplasmic compartments. Along this pathway, multiple pre-ribosomal particles are generated, which transiently associate with numerous non-ribosomal factors before mature 60S and 40S subunits are formed. However, most mechanistic details of ribosome biogenesis are still unknown. Here we identify a maturation step of the yeast pre-40S subunit that is regulated by the protein kinase Hrr25 and involves ribosomal protein Rps3. A high salt concentration releases Rps3 from isolated pre-40S particles but not from mature 40S subunits. Electron microscopy indicates that pre-40S particles lack a structural landmark present in mature 40S subunits, the 'beak'. The beak is formed by the protrusion of 18S ribosomal RNA helix 33, which is in close vicinity to Rps3. Two protein kinases Hrr25 and Rio2 are associated with pre-40S particles. Hrr25 phosphorylates Rps3 and the 40S synthesis factor Enp1. Phosphorylated Rsp3 and Enp1 readily dissociate from the pre-ribosome, whereas subsequent dephosphorylation induces formation of the beak structure and salt-resistant integration of Rps3 into the 40S subunit. In vivo depletion of Hrr25 inhibits growth and leads to the accumulation of immature 40S subunits that contain unstably bound Rps3. We conclude that the kinase activity of Hrr25 regulates the maturation of 40S ribosomal subunits.

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Year:  2006        PMID: 16738661     DOI: 10.1038/nature04840

Source DB:  PubMed          Journal:  Nature        ISSN: 0028-0836            Impact factor:   49.962


  116 in total

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Review 4.  Paradigms of ribosome synthesis: Lessons learned from ribosomal proteins.

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Review 5.  Specialized ribosomes: a new frontier in gene regulation and organismal biology.

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Review 8.  Powering through ribosome assembly.

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9.  Phosphorylation of right open reading frame 2 (Rio2) protein kinase by polo-like kinase 1 regulates mitotic progression.

Authors:  Ting Liu; Min Deng; Junhui Li; Xiaomei Tong; Qian Wei; Xin Ye
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10.  Proteomic and electron microscopy survey of large assemblies in macrophage cytoplasm.

Authors:  Bohumil Maco; Ian L Ross; Michael J Landsberg; Dmitri Mouradov; Neil F W Saunders; Ben Hankamer; Bostjan Kobe
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