Literature detail

Immune Escape Adaptive Mutations in the H7N9 Avian Influenza Hemagglutinin Protein Increase Virus Replication Fitness and Decrease Pandemic Potential.

Pengxiang Chang¹ Joshua E Sealy¹ Jean-Remy Sadeyen¹ Sushant Bhat¹ Deimante Lukosaityte¹ Yipeng Sun² Munir Iqbal³

Affiliations 3 institutions

The Pirbright Institute, Pirbright, United Kingdom.
College of Veterinary Medicine, China Agricultural University, Beijing, China.
The Pirbright Institute, Pirbright, United Kingdom [email protected].

PMID 32699084 2020 J Virol eng epublish

Article

Publication summary

H7N9 avian influenza viruses (AIVs) continue to evolve and remain a huge threat to human health and the poultry industry. Previously, serially passaging the H7N9 A/Anhui/1/2013 virus in the presence of homologous ferret antiserum resulted in immune escape viruses containing amino acid substitutions alanine to threonine at residues 125 (A125T) and 151 (A151T) and leucine to glutamine at residue 217 (L217Q) in the hemagglutinin (HA) protein. These HA mutations have also been found in field isolates in 2019. To investigate the potential threat of serum escape mutant viruses to humans and poultry, the impact of these HA substitutions, either individually or in combination, on receptor binding, pH of fusion, thermal stability, and virus replication were investigated. Our results showed the serum escape mutant formed large plaques in Madin-Darby canine kidney (MDCK) cells and grew robustly in vitro and in ovo They had a lower pH of fusion and increased thermal stability. Of note, the serum escape mutant completely lost the ability to bind to human-like receptor analogues. Further analysis revealed that N-linked glycosylation, as a result of A125T or A151T substitutions in HA, resulted in reduced receptor-binding avidity toward both human and avian-like receptor analogues, and the A125T+A151T mutations completely abolished human-like receptor binding. The L217Q mutation enhanced the H7N9 acid and thermal stability while the A151T mutation dramatically decreased H7N9 HA thermal stability. To conclude, H7N9 AIVs that contain A125T+A151T+L217Q mutations in the HA protein may pose a reduced pandemic risk but remain a heightened threat for poultry.IMPORTANCE Avian influenza H7N9 viruses have been causing disease outbreaks in poultry and humans. We previously determined that propagation of H7N9 virus in virus-specific antiserum gives rise to mutant viruses carrying mutations A125T+A151T+L217Q in their hemagglutinin protein, enabling the virus to overcome vaccine-induced immunity. As predicted, these immune escape mutations were also observed in the field viruses that likely emerged in the immunized or naturally exposed birds. This study demonstrates that the immune escape mutants also (i) gained greater replication ability in cultured cells and in chicken embryos as well as (ii) increased acid and thermal stability but (iii) lost preferences for binding to human-type receptor while maintaining binding for the avian-like receptor. Therefore, they potentially pose reduced pandemic risk. However, the emergent virus variants containing the indicated mutations remain a significant risk to poultry due to antigenic drift and improved fitness for poultry.

avian viruses H7N9 immune escape influenza poultry replication fitness zoonotic infections Mutation Pandemics Amino Acid Substitution Animals Dogs Hemagglutinins, Viral Hydrogen-Ion Concentration Influenza A Virus, H7N9 Subtype Influenza in Birds Madin Darby Canine Kidney Cells Models, Molecular

Structured evidence records

Evidence records

3 total

Receptor Usage 2 records

Receptor Usage Extraction confidence 0.95

Key finding

H7N9 influenza viruses with HA mutations A125T and A151T lose binding to human-like receptors and show reduced avidity for both avian and human receptor analogues, indicating altered receptor specificity.

Virus

Host

Location

Supporting text

The serum escape mutant completely lost the ability to bind to human-like receptor analogues. Further analysis revealed that N-linked glycosylation, as a result of A125T or A151T substitutions in HA, resulted in reduced receptor-binding avidity toward both human and avian-like receptor analogues, and the A125T+A151T mutations completely abolished human-like receptor binding.

Method: receptor-binding assay
Receptors: human-like receptor analogues

Receptor Usage Extraction confidence 0.95

Key finding

A125T and A151T substitutions in H7N9 HA reduce binding avidity toward avian-like receptors, suggesting decreased affinity and altered receptor usage.

Virus

Host

Location

Supporting text

Further analysis revealed that N-linked glycosylation, as a result of A125T or A151T substitutions in HA, resulted in reduced receptor-binding avidity toward both human and avian-like receptor analogues.

Method: receptor-binding assay
Receptors: avian-like receptor analogues

Molecular Adaptation 1 records

Molecular Adaptation Extraction confidence 1.00

Key finding

H7N9 avian influenza viruses possessing HA mutations A125T, A151T, and L217Q exhibit immune escape, enhanced replication fitness, improved stability, and altered receptor-binding specificity that reduce human-type receptor binding but favor avian adaptation.

Virus

Host

Location

Supporting text

Serial passaging of the H7N9 A/Anhui/1/2013 virus in the presence of homologous ferret antiserum resulted in viruses containing amino acid substitutions A125T, A151T, and L217Q in the hemagglutinin (HA) protein. These mutations altered receptor binding and increased acid and thermal stability. The mutants grew robustly in vitro and in ovo, lost the ability to bind human-like receptor analogues, and maintained avian-like receptor binding.

Genes or proteins: hemagglutinin; HA
Receptors: human-like receptor analogues; avian-like receptor analogues
Mutations: A125T; A151T; L217Q
Mechanism types: immune_escape; receptor_binding; replication_fitness; thermal_stability; acid_stability

Citation context

References

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Evidence overview

Evidence 3

Types 2

Virus 1

Host 2

Evidence types

Receptor Usage 2 Molecular Adaptation 1

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Publication metadata

Journal: Journal of virology
Volume / Issue / Pages: 94 / 19 / -
ISSN: 1098-5514
Journal country: United States
DOI: 10.1128/JVI.00216-20