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The Translation of Non-Canonical Open Reading Frames Controls Mucosal Immunity

The annotation of the mammalian protein coding genome is incomplete. Arbitrary open reading frame (ORF) size restriction and the absolute requirement for a methionine codon as the sole initiator of translation, have constrained identification of potentially important transcripts with non-canonical p...

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Autores principales: Jackson, Ruaidhrí, Kroehling, Lina, Khitun, Alexandra, Bailis, Will, Jarret, Abigail, York, Autumn G., Khan, Omair M., Brewer, J. Richard, Skadow, Mathias H., Duizer, Coco, Harman, Christian C. D., Chang, Lelina, Bielecki, Piotr, Solis, Angel G., Steach, Holly R., Slavoff, Sarah, Flavell, Richard A.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: 2018
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6939389/
https://www.ncbi.nlm.nih.gov/pubmed/30542152
http://dx.doi.org/10.1038/s41586-018-0794-7
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author Jackson, Ruaidhrí
Kroehling, Lina
Khitun, Alexandra
Bailis, Will
Jarret, Abigail
York, Autumn G.
Khan, Omair M.
Brewer, J. Richard
Skadow, Mathias H.
Duizer, Coco
Harman, Christian C. D.
Chang, Lelina
Bielecki, Piotr
Solis, Angel G.
Steach, Holly R.
Slavoff, Sarah
Flavell, Richard A.
author_facet Jackson, Ruaidhrí
Kroehling, Lina
Khitun, Alexandra
Bailis, Will
Jarret, Abigail
York, Autumn G.
Khan, Omair M.
Brewer, J. Richard
Skadow, Mathias H.
Duizer, Coco
Harman, Christian C. D.
Chang, Lelina
Bielecki, Piotr
Solis, Angel G.
Steach, Holly R.
Slavoff, Sarah
Flavell, Richard A.
author_sort Jackson, Ruaidhrí
collection PubMed
description The annotation of the mammalian protein coding genome is incomplete. Arbitrary open reading frame (ORF) size restriction and the absolute requirement for a methionine codon as the sole initiator of translation, have constrained identification of potentially important transcripts with non-canonical protein coding potential(1,2). Using unbiased transcriptomic approaches in macrophages responding to bacterial infection, we show widespread ribosome association with a large number of RNAs that were previously annotated as “non-protein coding”. Although the ability of such non-canonical ORFs to encode functional protein is controversial(3,4), we identify a plethora of novel short and non-ATG initiated ORFs with the ability to generate stable and spatially distinct proteins. Importantly, we show that the translation of a novel ORF ‘hidden’ within the long non-coding RNA Aw112010 is essential for the orchestration of mucosal immunity during both bacterial infection and colitis. Together this work expands our interpretation of the protein coding genome and demonstrates the critical nature of proteinaceous products generated from non-canonical ORFs to the immune response in vivo. We therefore propose that the misannotation of non-canonical ORF-containing genes as non-coding RNAs may obscure the essential role of a multitude of previously undiscovered protein coding genes in immunity and disease.
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spelling pubmed-69393892020-01-02 The Translation of Non-Canonical Open Reading Frames Controls Mucosal Immunity Jackson, Ruaidhrí Kroehling, Lina Khitun, Alexandra Bailis, Will Jarret, Abigail York, Autumn G. Khan, Omair M. Brewer, J. Richard Skadow, Mathias H. Duizer, Coco Harman, Christian C. D. Chang, Lelina Bielecki, Piotr Solis, Angel G. Steach, Holly R. Slavoff, Sarah Flavell, Richard A. Nature Article The annotation of the mammalian protein coding genome is incomplete. Arbitrary open reading frame (ORF) size restriction and the absolute requirement for a methionine codon as the sole initiator of translation, have constrained identification of potentially important transcripts with non-canonical protein coding potential(1,2). Using unbiased transcriptomic approaches in macrophages responding to bacterial infection, we show widespread ribosome association with a large number of RNAs that were previously annotated as “non-protein coding”. Although the ability of such non-canonical ORFs to encode functional protein is controversial(3,4), we identify a plethora of novel short and non-ATG initiated ORFs with the ability to generate stable and spatially distinct proteins. Importantly, we show that the translation of a novel ORF ‘hidden’ within the long non-coding RNA Aw112010 is essential for the orchestration of mucosal immunity during both bacterial infection and colitis. Together this work expands our interpretation of the protein coding genome and demonstrates the critical nature of proteinaceous products generated from non-canonical ORFs to the immune response in vivo. We therefore propose that the misannotation of non-canonical ORF-containing genes as non-coding RNAs may obscure the essential role of a multitude of previously undiscovered protein coding genes in immunity and disease. 2018-12-12 2018-12 /pmc/articles/PMC6939389/ /pubmed/30542152 http://dx.doi.org/10.1038/s41586-018-0794-7 Text en Users may view, print, copy, and download text and data-mine the content in such documents, for the purposes of academic research, subject always to the full Conditions of use:http://www.nature.com/authors/editorial_policies/license.html#terms
spellingShingle Article
Jackson, Ruaidhrí
Kroehling, Lina
Khitun, Alexandra
Bailis, Will
Jarret, Abigail
York, Autumn G.
Khan, Omair M.
Brewer, J. Richard
Skadow, Mathias H.
Duizer, Coco
Harman, Christian C. D.
Chang, Lelina
Bielecki, Piotr
Solis, Angel G.
Steach, Holly R.
Slavoff, Sarah
Flavell, Richard A.
The Translation of Non-Canonical Open Reading Frames Controls Mucosal Immunity
title The Translation of Non-Canonical Open Reading Frames Controls Mucosal Immunity
title_full The Translation of Non-Canonical Open Reading Frames Controls Mucosal Immunity
title_fullStr The Translation of Non-Canonical Open Reading Frames Controls Mucosal Immunity
title_full_unstemmed The Translation of Non-Canonical Open Reading Frames Controls Mucosal Immunity
title_short The Translation of Non-Canonical Open Reading Frames Controls Mucosal Immunity
title_sort translation of non-canonical open reading frames controls mucosal immunity
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6939389/
https://www.ncbi.nlm.nih.gov/pubmed/30542152
http://dx.doi.org/10.1038/s41586-018-0794-7
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