Translation Initiation by Factor-independent Binding of Eukaryotic Ribosomes to Internal Ribosomal Entry Sites

Overview

Journal C R Biol

Specialty Biology

Date 2005 Jul 5

PMID 15992743

Citations 60

Authors

Andrey V Pisarev

Nikolay E Shirokikh

Christopher U T Hellen

Affiliations

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Abstract

Two exceptional mechanisms of eukaryotic translation initiation have recently been identified that differ fundamentally from the canonical factor-mediated, end-dependent mechanism of ribosomal attachment to mRNA. Instead, ribosomal 40S subunits bind in a factor-independent manner to the internal ribosomal entry site (IRES) in an mRNA. These two mechanisms are exemplified by initiation on the unrelated approximately 300 nt.-long Hepatitis C virus (HCV) IRES and the approximately 200 nt.-long cricket paralysis virus (CrPV) intergenic region (IGR) IRES, respectively. Ribosomal binding involves interaction with multiple non-contiguous sites on these IRESs, and therefore also differs from the factor-independent attachment of prokaryotic ribosomes to mRNA, which involves base-pairing to the linear Shine-Dalgarno sequence. The HCV IRES binds to the solvent side of the 40S subunit, docks a domain of the IRES into the ribosomal exit (E) site and places the initiation codon in the ribosomal peptidyl (P) site. Subsequent binding of eIF3 and the eIF2-GTP/initiator tRNA complex to form a 48S complex is followed by subunit joining to form an 80S ribosome. The CrPV IRES binds to ribosomes in a very different manner, by occupying the ribosomal E and P sites in the intersubunit cavity, thereby excluding initiator tRNA. Ribosomes enter the elongation stage of translation directly, without any involvement of initiator tRNA or initiation factors, following recruitment of aminoacyl-tRNA to the ribosomal aminoacyl (A) site and translocation of it to the P site.

Citing Articles

Editorial: RNA machines.

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Short and Sweet: Viral 5`-UTR as a Canonical and Non-Canonical Translation Initiation Switch.

Trainor B, Shcherbik N J Cell Immunol. 2022; 3(5):296-304.

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A Retrospective on eIF2A-and Not the Alpha Subunit of eIF2.

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Regulation of the Transferrin Receptor Recycling in Hepatitis C Virus-Replicating Cells.

Haberger V, Elgner F, Roos J, Bender D, Hildt E Front Cell Dev Biol. 2020; 8:44.

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The Israeli acute paralysis virus IRES captures host ribosomes by mimicking a ribosomal state with hybrid tRNAs.

Acosta-Reyes F, Neupane R, Frank J, Fernandez I EMBO J. 2019; 38(21):e102226.

PMID: 31609474 PMC: 6826211. DOI: 10.15252/embj.2019102226.