Literature DB >> 29100052

Structural Basis for Polyproline-Mediated Ribosome Stalling and Rescue by the Translation Elongation Factor EF-P.

Paul Huter1, Stefan Arenz1, Lars V Bock2, Michael Graf1, Jan Ole Frister3, Andre Heuer1, Lauri Peil4, Agata L Starosta1, Ingo Wohlgemuth3, Frank Peske3, Jiří Nováček5, Otto Berninghausen1, Helmut Grubmüller2, Tanel Tenson4, Roland Beckmann1, Marina V Rodnina3, Andrea C Vaiana2, Daniel N Wilson6.   

Abstract

Ribosomes synthesizing proteins containing consecutive proline residues become stalled and require rescue via the action of uniquely modified translation elongation factors, EF-P in bacteria, or archaeal/eukaryotic a/eIF5A. To date, no structures exist of EF-P or eIF5A in complex with translating ribosomes stalled at polyproline stretches, and thus structural insight into how EF-P/eIF5A rescue these arrested ribosomes has been lacking. Here we present cryo-EM structures of ribosomes stalled on proline stretches, without and with modified EF-P. The structures suggest that the favored conformation of the polyproline-containing nascent chain is incompatible with the peptide exit tunnel of the ribosome and leads to destabilization of the peptidyl-tRNA. Binding of EF-P stabilizes the P-site tRNA, particularly via interactions between its modification and the CCA end, thereby enforcing an alternative conformation of the polyproline-containing nascent chain, which allows a favorable substrate geometry for peptide bond formation.
Copyright © 2017 Elsevier Inc. All rights reserved.

Entities:  

Keywords:  EF-P; RNA; a-IF5A; eIF5A; nascent chain; prolines; ribosome; single particle cryo-EM; stalling; translation elongation

Mesh:

Substances:

Year:  2017        PMID: 29100052     DOI: 10.1016/j.molcel.2017.10.014

Source DB:  PubMed          Journal:  Mol Cell        ISSN: 1097-2765            Impact factor:   17.970


  42 in total

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9.  Controlling orthogonal ribosome subunit interactions enables evolution of new function.

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