Translation initiation factors eIF3 and HCR1 control translation termination and stop codon read-through in yeast cells.

Translation initiation factors eIF3 and HCR1 control translation termination and stop codon read-through in yeast cells.

Translation is divided into initiation, elongation, termination and ribosome recycling. Earlier work implicated several eukaryotic initiation factors (eIFs) in ribosomal recycling in vitro. Here, we uncover roles for HCR1 and eIF3 in translation termination in vivo. A substantial proportion of eIF3,...

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Main Authors: Petra Beznosková, Lucie Cuchalová, Susan Wagner, Christopher J Shoemaker, Stanislava Gunišová, Tobias von der Haar, Leoš Shivaya Valášek
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2013-11-01
Series:PLoS Genetics
Online Access:http://europepmc.org/articles/PMC3836723?pdf=render
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spelling doaj-3858d747f4b14c1c979c3375267be6982020-11-25T01:19:27ZengPublic Library of Science (PLoS)PLoS Genetics1553-73901553-74042013-11-01911e100396210.1371/journal.pgen.1003962Translation initiation factors eIF3 and HCR1 control translation termination and stop codon read-through in yeast cells.Petra BeznoskováLucie CuchalováSusan WagnerChristopher J ShoemakerStanislava GunišováTobias von der HaarLeoš Shivaya ValášekTranslation is divided into initiation, elongation, termination and ribosome recycling. Earlier work implicated several eukaryotic initiation factors (eIFs) in ribosomal recycling in vitro. Here, we uncover roles for HCR1 and eIF3 in translation termination in vivo. A substantial proportion of eIF3, HCR1 and eukaryotic release factor 3 (eRF3) but not eIF5 (a well-defined "initiation-specific" binding partner of eIF3) specifically co-sediments with 80S couples isolated from RNase-treated heavy polysomes in an eRF1-dependent manner, indicating the presence of eIF3 and HCR1 on terminating ribosomes. eIF3 and HCR1 also occur in ribosome- and RNA-free complexes with both eRFs and the recycling factor ABCE1/RLI1. Several eIF3 mutations reduce rates of stop codon read-through and genetically interact with mutant eRFs. In contrast, a slow growing deletion of hcr1 increases read-through and accumulates eRF3 in heavy polysomes in a manner suppressible by overexpressed ABCE1/RLI1. Based on these and other findings we propose that upon stop codon recognition, HCR1 promotes eRF3·GDP ejection from the post-termination complexes to allow binding of its interacting partner ABCE1/RLI1. Furthermore, the fact that high dosage of ABCE1/RLI1 fully suppresses the slow growth phenotype of hcr1Δ as well as its termination but not initiation defects implies that the termination function of HCR1 is more critical for optimal proliferation than its function in translation initiation. Based on these and other observations we suggest that the assignment of HCR1 as a bona fide eIF3 subunit should be reconsidered. Together our work characterizes novel roles of eIF3 and HCR1 in stop codon recognition, defining a communication bridge between the initiation and termination/recycling phases of translation.http://europepmc.org/articles/PMC3836723?pdf=render
collection DOAJ
language English
format Article
sources DOAJ
author Petra Beznosková
Lucie Cuchalová
Susan Wagner
Christopher J Shoemaker
Stanislava Gunišová
Tobias von der Haar
Leoš Shivaya Valášek
spellingShingle Petra Beznosková
Lucie Cuchalová
Susan Wagner
Christopher J Shoemaker
Stanislava Gunišová
Tobias von der Haar
Leoš Shivaya Valášek
Translation initiation factors eIF3 and HCR1 control translation termination and stop codon read-through in yeast cells.
PLoS Genetics
author_facet Petra Beznosková
Lucie Cuchalová
Susan Wagner
Christopher J Shoemaker
Stanislava Gunišová
Tobias von der Haar
Leoš Shivaya Valášek
author_sort Petra Beznosková
title Translation initiation factors eIF3 and HCR1 control translation termination and stop codon read-through in yeast cells.
title_short Translation initiation factors eIF3 and HCR1 control translation termination and stop codon read-through in yeast cells.
title_full Translation initiation factors eIF3 and HCR1 control translation termination and stop codon read-through in yeast cells.
title_fullStr Translation initiation factors eIF3 and HCR1 control translation termination and stop codon read-through in yeast cells.
title_full_unstemmed Translation initiation factors eIF3 and HCR1 control translation termination and stop codon read-through in yeast cells.
title_sort translation initiation factors eif3 and hcr1 control translation termination and stop codon read-through in yeast cells.
publisher Public Library of Science (PLoS)
series PLoS Genetics
issn 1553-7390
1553-7404
publishDate 2013-11-01
description Translation is divided into initiation, elongation, termination and ribosome recycling. Earlier work implicated several eukaryotic initiation factors (eIFs) in ribosomal recycling in vitro. Here, we uncover roles for HCR1 and eIF3 in translation termination in vivo. A substantial proportion of eIF3, HCR1 and eukaryotic release factor 3 (eRF3) but not eIF5 (a well-defined "initiation-specific" binding partner of eIF3) specifically co-sediments with 80S couples isolated from RNase-treated heavy polysomes in an eRF1-dependent manner, indicating the presence of eIF3 and HCR1 on terminating ribosomes. eIF3 and HCR1 also occur in ribosome- and RNA-free complexes with both eRFs and the recycling factor ABCE1/RLI1. Several eIF3 mutations reduce rates of stop codon read-through and genetically interact with mutant eRFs. In contrast, a slow growing deletion of hcr1 increases read-through and accumulates eRF3 in heavy polysomes in a manner suppressible by overexpressed ABCE1/RLI1. Based on these and other findings we propose that upon stop codon recognition, HCR1 promotes eRF3·GDP ejection from the post-termination complexes to allow binding of its interacting partner ABCE1/RLI1. Furthermore, the fact that high dosage of ABCE1/RLI1 fully suppresses the slow growth phenotype of hcr1Δ as well as its termination but not initiation defects implies that the termination function of HCR1 is more critical for optimal proliferation than its function in translation initiation. Based on these and other observations we suggest that the assignment of HCR1 as a bona fide eIF3 subunit should be reconsidered. Together our work characterizes novel roles of eIF3 and HCR1 in stop codon recognition, defining a communication bridge between the initiation and termination/recycling phases of translation.
url http://europepmc.org/articles/PMC3836723?pdf=render
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