Published December 30, 2021 | Version v1
Journal article Open

Mutations in the genomes of avian influenza viruses of the H1 and H5 subtypes responsible for adaptation to mammals

  • 1. National Research Center for Epidemiology and Microbiology named after N. F. Gamaleya, 18, Gamaleya str., Moscow, 123098, Russia
  • 2. National Research Center for Epidemiology and Microbiology named after N. F. Gamaleya, 18, Gamaleya str., Moscow, 123098, Russia; I. M. Sechenov First Moscow State University, 2/62, Lomonosov pr., Moscow, 101000, Russia
  • 3. All-Russian Institute for Scientific and Technical Information of the Russian Academy of Sciences, 20, Usievicha str., Москва, 125315, Russia

Description

Avian influenza viruses of the H1 and H5 subtypes were involved in the formation of highly pathogenic viruses that caused pandemics and panzootics in the 20th–21st centuries. In order to assess the zoonotic potential of viruses of these subtypes, two viruses of the H1N1 and H5N3 subtypes have been isolated from wild ducks in Moscow and adapted for growth in mouse lungs. Their phenotypic properties were studied, and the genetic changes that occurred during adaptation were identified. The original A/duck/Moscow/4970/2013 (H1N1) and A/duck/Moscow/4182-C/2010 (H5N3) viruses were apathogenic for mice but became pathogenic after 7–10 passages in mouse lungs. Complete genome sequencing revealed 2 amino acid substitutions in the proteins of the H1N1 mouse-adapted variant (Glu627Lys in PB2 and Asp35Asn in hemagglutinin (HA) – numbering according to H3) and 6 mutations in the proteins of H5N3 virus (Glu627lys in PB2, Val113Ala in PB1, Ser82Pro in PB1-F2, Lys52Arg in HA2, Arg65Lys in NP, and Ser59Ile in NA). The increase in virulence is most likely due to a Glu627Lys substitution in the protein PB2 found in both viruses. The replacement Asp35Asn in HA of the mouse-adapted H1N1 virus is associated with an increase in the pH value of the HA transition to 5.5 versus 5.0 for that of the wild virus. The mutations found in the HA, NA, and PB1-F2 proteins of the adapted H5N3 variant are unique. The mutations Glu627Lys in PB2, Arg65Lys in NP, and Val113Ala in PB1 are most likely host adaptive.

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