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Translation initiation downstream from annotated start codons in human mRNAs coevolves with the Kozak context

Eukaryotic translation initiation involves preinitiation ribosomal complex 5′-to-3′ directional probing of mRNA for codons suitable for starting protein synthesis. The recognition of codons as starts depends on the codon identity and on its immediate nucleotide context known as Kozak context. When t...

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Autores principales: Benitez-Cantos, Maria S., Yordanova, Martina M., O'Connor, Patrick B.F., Zhdanov, Alexander V., Kovalchuk, Sergey I., Papkovsky, Dmitri B., Andreev, Dmitry E., Baranov, Pavel V.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Cold Spring Harbor Laboratory Press 2020
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7397870/
https://www.ncbi.nlm.nih.gov/pubmed/32669370
http://dx.doi.org/10.1101/gr.257352.119
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author Benitez-Cantos, Maria S.
Yordanova, Martina M.
O'Connor, Patrick B.F.
Zhdanov, Alexander V.
Kovalchuk, Sergey I.
Papkovsky, Dmitri B.
Andreev, Dmitry E.
Baranov, Pavel V.
author_facet Benitez-Cantos, Maria S.
Yordanova, Martina M.
O'Connor, Patrick B.F.
Zhdanov, Alexander V.
Kovalchuk, Sergey I.
Papkovsky, Dmitri B.
Andreev, Dmitry E.
Baranov, Pavel V.
author_sort Benitez-Cantos, Maria S.
collection PubMed
description Eukaryotic translation initiation involves preinitiation ribosomal complex 5′-to-3′ directional probing of mRNA for codons suitable for starting protein synthesis. The recognition of codons as starts depends on the codon identity and on its immediate nucleotide context known as Kozak context. When the context is weak (i.e., nonoptimal), leaky scanning takes place during which a fraction of ribosomes continues the mRNA probing. We explored the relationship between the context of AUG codons annotated as starts of protein-coding sequences and the next AUG codon occurrence. We found that AUG codons downstream from weak starts occur in the same frame more frequently than downstream from strong starts. We suggest that evolutionary selection on in-frame AUGs downstream from weak start codons is driven by the advantage of the reduction of wasteful out-of-frame product synthesis and also by the advantage of producing multiple proteoforms from certain mRNAs. We confirmed translation initiation downstream from weak start codons using ribosome profiling data. We also tested translation of alternative start codons in 10 specific human genes using reporter constructs. In all tested cases, initiation at downstream start codons was more productive than at the annotated ones. In most cases, optimization of Kozak context did not completely abolish downstream initiation, and in the specific example of CMPK1 mRNA, the optimized start remained unproductive. Collectively, our work reveals previously uncharacterized forces shaping the evolution of protein-coding genes and points to the plurality of translation initiation and the existence of sequence features influencing start codon selection, other than Kozak context.
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spelling pubmed-73978702020-08-13 Translation initiation downstream from annotated start codons in human mRNAs coevolves with the Kozak context Benitez-Cantos, Maria S. Yordanova, Martina M. O'Connor, Patrick B.F. Zhdanov, Alexander V. Kovalchuk, Sergey I. Papkovsky, Dmitri B. Andreev, Dmitry E. Baranov, Pavel V. Genome Res Research Eukaryotic translation initiation involves preinitiation ribosomal complex 5′-to-3′ directional probing of mRNA for codons suitable for starting protein synthesis. The recognition of codons as starts depends on the codon identity and on its immediate nucleotide context known as Kozak context. When the context is weak (i.e., nonoptimal), leaky scanning takes place during which a fraction of ribosomes continues the mRNA probing. We explored the relationship between the context of AUG codons annotated as starts of protein-coding sequences and the next AUG codon occurrence. We found that AUG codons downstream from weak starts occur in the same frame more frequently than downstream from strong starts. We suggest that evolutionary selection on in-frame AUGs downstream from weak start codons is driven by the advantage of the reduction of wasteful out-of-frame product synthesis and also by the advantage of producing multiple proteoforms from certain mRNAs. We confirmed translation initiation downstream from weak start codons using ribosome profiling data. We also tested translation of alternative start codons in 10 specific human genes using reporter constructs. In all tested cases, initiation at downstream start codons was more productive than at the annotated ones. In most cases, optimization of Kozak context did not completely abolish downstream initiation, and in the specific example of CMPK1 mRNA, the optimized start remained unproductive. Collectively, our work reveals previously uncharacterized forces shaping the evolution of protein-coding genes and points to the plurality of translation initiation and the existence of sequence features influencing start codon selection, other than Kozak context. Cold Spring Harbor Laboratory Press 2020-07 /pmc/articles/PMC7397870/ /pubmed/32669370 http://dx.doi.org/10.1101/gr.257352.119 Text en © 2020 Benitez-Cantos et al.; Published by Cold Spring Harbor Laboratory Press http://creativecommons.org/licenses/by/4.0/ This article, published in Genome Research, is available under a Creative Commons License (Attribution 4.0 International), as described at http://creativecommons.org/licenses/by/4.0/.
spellingShingle Research
Benitez-Cantos, Maria S.
Yordanova, Martina M.
O'Connor, Patrick B.F.
Zhdanov, Alexander V.
Kovalchuk, Sergey I.
Papkovsky, Dmitri B.
Andreev, Dmitry E.
Baranov, Pavel V.
Translation initiation downstream from annotated start codons in human mRNAs coevolves with the Kozak context
title Translation initiation downstream from annotated start codons in human mRNAs coevolves with the Kozak context
title_full Translation initiation downstream from annotated start codons in human mRNAs coevolves with the Kozak context
title_fullStr Translation initiation downstream from annotated start codons in human mRNAs coevolves with the Kozak context
title_full_unstemmed Translation initiation downstream from annotated start codons in human mRNAs coevolves with the Kozak context
title_short Translation initiation downstream from annotated start codons in human mRNAs coevolves with the Kozak context
title_sort translation initiation downstream from annotated start codons in human mrnas coevolves with the kozak context
topic Research
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7397870/
https://www.ncbi.nlm.nih.gov/pubmed/32669370
http://dx.doi.org/10.1101/gr.257352.119
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