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SARS-CoV-2 mRNA vaccine is re-adenylated in vivo, enhancing antigen production and immune response

View ORCID ProfilePaweł S Krawczyk, View ORCID ProfileOlga Gewartowska, View ORCID ProfileMichał Mazur, View ORCID ProfileWiktoria Orzeł, View ORCID ProfileKatarzyna Matylla-Kulińska, Sebastian Jeleń, Paweł Turowski, Tomasz Śpiewla, View ORCID ProfileBartosz Tarkowski, View ORCID ProfileAgnieszka Tudek, View ORCID ProfileAleksandra Brouze, Aleksandra Wesołowska, View ORCID ProfileDominika Nowis, View ORCID ProfileJakub Gołąb, View ORCID ProfileJoanna Kowalska, View ORCID ProfileJacek Jemielity, View ORCID ProfileAndrzej Dziembowski, View ORCID ProfileSeweryn Mroczek
doi: https://doi.org/10.1101/2022.12.01.518149
Paweł S Krawczyk
1International Institute of Molecular and Cell Biology, 4 Ks. Trojdena, 02-106 Warsaw, Poland
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  • ORCID record for Paweł S Krawczyk
Olga Gewartowska
1International Institute of Molecular and Cell Biology, 4 Ks. Trojdena, 02-106 Warsaw, Poland
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  • ORCID record for Olga Gewartowska
Michał Mazur
1International Institute of Molecular and Cell Biology, 4 Ks. Trojdena, 02-106 Warsaw, Poland
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Wiktoria Orzeł
1International Institute of Molecular and Cell Biology, 4 Ks. Trojdena, 02-106 Warsaw, Poland
2Faculty of Biology, University of Warsaw, 5a Pawinskiego, 02-106, Warsaw, Poland
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Katarzyna Matylla-Kulińska
1International Institute of Molecular and Cell Biology, 4 Ks. Trojdena, 02-106 Warsaw, Poland
2Faculty of Biology, University of Warsaw, 5a Pawinskiego, 02-106, Warsaw, Poland
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Sebastian Jeleń
1International Institute of Molecular and Cell Biology, 4 Ks. Trojdena, 02-106 Warsaw, Poland
2Faculty of Biology, University of Warsaw, 5a Pawinskiego, 02-106, Warsaw, Poland
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Paweł Turowski
3ExploRNA Therapeutics, 101 Żwirki i Wigury, 02-089, Warsaw, Poland
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Tomasz Śpiewla
4Faculty of Physics, University of Warsaw, Pasteura 5, 02-093, Warsaw, Poland
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Bartosz Tarkowski
1International Institute of Molecular and Cell Biology, 4 Ks. Trojdena, 02-106 Warsaw, Poland
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Agnieszka Tudek
5Institute of Biochemistry and Biophysics, 5A Pawińskiego, 02-106 Warsaw, Poland
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Aleksandra Brouze
1International Institute of Molecular and Cell Biology, 4 Ks. Trojdena, 02-106 Warsaw, Poland
2Faculty of Biology, University of Warsaw, 5a Pawinskiego, 02-106, Warsaw, Poland
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Aleksandra Wesołowska
6Department of Medical Biology, Medical University of Warsaw, Madalinskiego 25, 02-455, Warsaw, Poland
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Dominika Nowis
7Department of Immunology, Medical University of Warsaw, 5 Nielubowicza Str., 02-097, Warsaw, Poland
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  • ORCID record for Dominika Nowis
Jakub Gołąb
7Department of Immunology, Medical University of Warsaw, 5 Nielubowicza Str., 02-097, Warsaw, Poland
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Joanna Kowalska
4Faculty of Physics, University of Warsaw, Pasteura 5, 02-093, Warsaw, Poland
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Jacek Jemielity
8Centre of New Technologies, University of Warsaw, Banacha 2c, 02-097, Warsaw, Poland
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Andrzej Dziembowski
1International Institute of Molecular and Cell Biology, 4 Ks. Trojdena, 02-106 Warsaw, Poland
2Faculty of Biology, University of Warsaw, 5a Pawinskiego, 02-106, Warsaw, Poland
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  • For correspondence: adziembowski@iimcb.gov.pl s.mroczek2@uw.edu.pl
Seweryn Mroczek
2Faculty of Biology, University of Warsaw, 5a Pawinskiego, 02-106, Warsaw, Poland
1International Institute of Molecular and Cell Biology, 4 Ks. Trojdena, 02-106 Warsaw, Poland
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  • For correspondence: adziembowski@iimcb.gov.pl s.mroczek2@uw.edu.pl
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Abstract

Though mRNA vaccines against COVID-19 have revolutionized vaccinology and have been administered in billions of doses, we know incredibly little about how mRNA vaccines are metabolized in vivo. Here we implemented enhanced nanopore Direct RNA sequencing (eDRS), to enable the analysis of single Moderna’s mRNA-1273 molecules, giving in vivo information about the sequence and poly(A) tails.

We show that mRNA-1273, with all uridines replaced by N1-methylpseudouridine (mΨ), is terminated by a long poly(A) tail (∼100 nucleotides) followed by an mΨCmΨAG sequence. In model cell lines, mRNA-1273 is swiftly degraded in a process initiated by the removal of mΨCmΨAG, followed by CCR4-NOT-mediated deadenylation. In contrast, intramuscularly inoculated mRNA-1273 undergoes more complex modifications. Notably, mRNA-1273 molecules are re-adenylated after mΨCmΨAG removal. Detailed analysis of immune cells involved in antigen production revealed that in macrophages, after mΨCmΨAG removal, vaccine mRNA is very efficiently re-adenylated, and poly(A) tails can reach up to 200A. In contrast, in dendritic cells, vaccine mRNA undergoes slow deadenylation-dependent decay. We further demonstrate that enhancement of mRNA stability in macrophages is mediated by TENT5 poly(A) polymerases, whose expression is induced by the vaccine itself. Lack of TENT5-mediated re-adenylation results in lower antigen production and severely compromises specific immunoglobulin production following vaccination.

Together, our findings provide an unexpected principle for the high efficacy of mRNA vaccines and open new possibilities for their improvement. They also emphasize that, in addition to targeting a protein of interest, the design of mRNA therapeutics should be customized to its cellular destination.

Competing Interest Statement

Jacek Jemielity, Joanna Kowalska, Jakub Golab, and Dominika Nowis are founders of ExploRNA Therapeutics and Pawel Turowski is an employee of ExploRNA Therapeutics.

Copyright 
The copyright holder for this preprint is the author/funder, who has granted bioRxiv a license to display the preprint in perpetuity. It is made available under a CC-BY-NC-ND 4.0 International license.
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Posted December 01, 2022.
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SARS-CoV-2 mRNA vaccine is re-adenylated in vivo, enhancing antigen production and immune response
Paweł S Krawczyk, Olga Gewartowska, Michał Mazur, Wiktoria Orzeł, Katarzyna Matylla-Kulińska, Sebastian Jeleń, Paweł Turowski, Tomasz Śpiewla, Bartosz Tarkowski, Agnieszka Tudek, Aleksandra Brouze, Aleksandra Wesołowska, Dominika Nowis, Jakub Gołąb, Joanna Kowalska, Jacek Jemielity, Andrzej Dziembowski, Seweryn Mroczek
bioRxiv 2022.12.01.518149; doi: https://doi.org/10.1101/2022.12.01.518149
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SARS-CoV-2 mRNA vaccine is re-adenylated in vivo, enhancing antigen production and immune response
Paweł S Krawczyk, Olga Gewartowska, Michał Mazur, Wiktoria Orzeł, Katarzyna Matylla-Kulińska, Sebastian Jeleń, Paweł Turowski, Tomasz Śpiewla, Bartosz Tarkowski, Agnieszka Tudek, Aleksandra Brouze, Aleksandra Wesołowska, Dominika Nowis, Jakub Gołąb, Joanna Kowalska, Jacek Jemielity, Andrzej Dziembowski, Seweryn Mroczek
bioRxiv 2022.12.01.518149; doi: https://doi.org/10.1101/2022.12.01.518149

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