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Potential coupling between SARS-CoV-2 replicative fitness and interactions of its nucleoprotein with human 14-3-3 proteins

Kristina V. Tugaeva, Andrey A. Sysoev, Jake L. R. Smith, View ORCID ProfileRichard B. Cooley, View ORCID ProfileAlfred A. Antson, View ORCID ProfileNikolai N. Sluchanko
doi: https://doi.org/10.1101/2021.12.23.474009
Kristina V. Tugaeva
1A.N. Bach Institute of Biochemistry, Federal Research Center of Biotechnology of the Russian Academy of Sciences, 119071, Moscow, Russia
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Andrey A. Sysoev
1A.N. Bach Institute of Biochemistry, Federal Research Center of Biotechnology of the Russian Academy of Sciences, 119071, Moscow, Russia
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Jake L. R. Smith
2York Structural Biology Laboratory, Department of Chemistry, University of York, York YO10 5DD, United Kingdom
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Richard B. Cooley
3Department of Biochemistry and Biophysics, Oregon State University, Corvallis, OR, 97331, USA
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Alfred A. Antson
2York Structural Biology Laboratory, Department of Chemistry, University of York, York YO10 5DD, United Kingdom
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  • For correspondence: nikolai.sluchanko@mail.ru fred.antson@york.ac.uk
Nikolai N. Sluchanko
1A.N. Bach Institute of Biochemistry, Federal Research Center of Biotechnology of the Russian Academy of Sciences, 119071, Moscow, Russia
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  • For correspondence: nikolai.sluchanko@mail.ru fred.antson@york.ac.uk
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Abstract

The SARS-CoV-2 nucleocapsid protein (N) is responsible for viral genome packaging and virion assembly. Being highly abundant in the host cell, N interacts with numerous human proteins and undergoes multisite phosphorylation in vivo. When phosphorylated within its Ser/Arg-rich region, a tract highly prone to mutations as exemplified in the Omicron and Delta variants, N recruits human 14-3-3 proteins, potentially hijacking their functions. Here, we show that in addition to phosphorylated Ser197, an alternative, less conserved phosphosite at Thr205 not found in SARS-CoV N binds 14-3-3 with micromolar affinity and is in fact preferred over pS197. Fluorescence anisotropy reveals a distinctive pT205/pS197 binding selectivity towards the seven human 14-3-3 isoforms. Crystal structures explain the structural basis for the discovered selectivity towards SARS-CoV-2 N phosphopeptides, and also enable prediction for how N variants interact with 14-3-3, suggesting a link between the strength of this interaction and replicative fitness of emerging coronavirus variants.

Competing Interest Statement

The authors have declared no competing interest.

Footnotes

  • Textual corrections, correction of the erroneous formatting of some special symbols during PDF conversion.

  • https://doi.org/10.2210/pdb7QIK/pdb

  • https://doi.org/10.2210/pdb7QIP/pdb

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 4.0 International license.
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Posted December 26, 2021.
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Potential coupling between SARS-CoV-2 replicative fitness and interactions of its nucleoprotein with human 14-3-3 proteins
Kristina V. Tugaeva, Andrey A. Sysoev, Jake L. R. Smith, Richard B. Cooley, Alfred A. Antson, Nikolai N. Sluchanko
bioRxiv 2021.12.23.474009; doi: https://doi.org/10.1101/2021.12.23.474009
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Potential coupling between SARS-CoV-2 replicative fitness and interactions of its nucleoprotein with human 14-3-3 proteins
Kristina V. Tugaeva, Andrey A. Sysoev, Jake L. R. Smith, Richard B. Cooley, Alfred A. Antson, Nikolai N. Sluchanko
bioRxiv 2021.12.23.474009; doi: https://doi.org/10.1101/2021.12.23.474009

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