Mutations Conferring Increased Sensitivity to Tripartite Motif 22 Restriction Accumulated Progressively in the Nucleoprotein of Seasonal Influenza A (H1N1) Viruses between 1918 and 2009

Isabel Pagani; Andrea Di Pietro; Alexandra Oteiza; Michela Ghitti; Nadir Mechti; Nadia Naffakh; Elisa Vicenzi

doi:10.1128/mSphere.00110-18

Mutations Conferring Increased Sensitivity to Tripartite Motif 22 Restriction Accumulated Progressively in the Nucleoprotein of Seasonal Influenza A (H1N1) Viruses between 1918 and 2009

mSphere. 2018 Apr 4;3(2):e00110-18. doi: 10.1128/mSphere.00110-18. Print 2018 Apr 25.

Authors

Isabel Pagani^#¹, Andrea Di Pietro^#¹, Alexandra Oteiza², Michela Ghitti¹, Nadir Mechti², Nadia Naffakh^{3

4

5}, Elisa Vicenzi⁶

Affiliations

¹ San Raffaele Scientific Institute, Milan, Italy.
² CNRS UMR 5235, DIMNP, University of Montpellier, Montpellier, France.
³ Institut Pasteur, Unité de Génétique Moléculaire des Virus à ARN, Département de Virologie, Paris, France.
⁴ CNRS, UMR3569, Paris, France.
⁵ Université Paris Diderot, Sorbonne Paris Cité, Paris, France.
⁶ San Raffaele Scientific Institute, Milan, Italy vicenzi.elisa@hsr.it.

^# Contributed equally.

Abstract

Influenza A viruses (IAVs) can cause zoonotic infections with pandemic potential when most of the human population is immunologically naive. After a pandemic, IAVs evolve to become seasonal in the human host by acquiring adaptive mutations. We have previously reported that the interferon (IFN)-inducible tripartite motif 22 (TRIM22) protein restricts the replication of seasonal IAVs by direct interaction with the viral nucleoprotein (NP), leading to its polyubiquitination and proteasomal degradation. Here we show that, in contrast to seasonal H1N1 IAVs, the 2009 pandemic H1N1 strain as well as H1N1 strains from the 1930s are resistant to TRIM22 restriction. We demonstrate that arginine-to-lysine substitutions conferring an increased sensitivity to TRIM22-dependent ubiquitination accumulated progressively in the NP of seasonal influenza A (H1N1) viruses between 1918 and 2009. Our findings suggest that during long-term circulation and evolution of IAVs in humans, adaptive mutations are favored at the expense of an increased sensitivity to some components of the innate immune response.IMPORTANCE We have uncovered that long-term circulation of seasonal influenza A viruses (IAV) in the human population resulted in the progressive acquisition of increased sensitivity to a component of the innate immune response: the type I interferon-inducible TRIM22 protein, which acts as a restriction factor by inducing the polyubiquitination of the IAV nucleoprotein (NP). We show that four arginine residues present in the NP of the 1918 H1N1 pandemic strain and early postpandemic strains were progressively substituted for by lysines between 1918 and 2009, rendering NP more susceptible to TRIM22-mediated ubiquitination. Our observations suggest that during long-term evolution of IAVs in humans, variants endowed with increased susceptibility to TRIM22 restriction emerge, highlighting the complexity of selection pressures acting on the NP.

Keywords: TRIM22; evolution; influenza A virus; nucleoprotein; restriction.

MeSH terms

Amino Acid Sequence
Amino Acid Substitution
Animals
Arginine / genetics
Dogs
Evolution, Molecular*
HEK293 Cells
Host-Pathogen Interactions
Humans
Immunity, Innate
Influenza A Virus, H1N1 Subtype / genetics*
Influenza, Human / virology
Lysine / genetics
Madin Darby Canine Kidney Cells
Minor Histocompatibility Antigens / metabolism*
Mutagenesis, Site-Directed
Mutation*
Nucleocapsid Proteins
Protein Structure, Tertiary
RNA-Binding Proteins / genetics*
Repressor Proteins / metabolism*
Tripartite Motif Proteins / metabolism*
Ubiquitin-Protein Ligases / metabolism
Ubiquitination
Viral Core Proteins / genetics*
Virus Replication

Substances

Minor Histocompatibility Antigens
NP protein, Influenza A virus
Nucleocapsid Proteins
RNA-Binding Proteins
Repressor Proteins
TRIM22 protein, human
Tripartite Motif Proteins
Viral Core Proteins
Arginine
Ubiquitin-Protein Ligases
Lysine