Literature detail

Receptor binding by a ferret-transmissible H5 avian influenza virus.

Xiaoli Xiong¹ Peter J Coombs Stephen R Martin Junfeng Liu Haixia Xiao John W McCauley Kathrin Locher Philip A Walker Patrick J Collins Yoshihiro Kawaoka John J Skehel Steven J Gamblin

Affiliations 1 institutions

MRC National Institute for Medical Research, The Ridgeway, Mill Hill, London NW7 1AA, UK.

PMID 23615615 2013 Nature eng ppublish

PubMed DOI Browse context

Article

Publication summary

Cell-surface-receptor binding by influenza viruses is a key determinant of their transmissibility, both from avian and animal species to humans as well as from human to human. Highly pathogenic avian H5N1 viruses that are a threat to public health have been observed to acquire affinity for human receptors, and transmissible-mutant-selection experiments have identified a virus that is transmissible in ferrets, the generally accepted experimental model for influenza in humans. Here, our quantitative biophysical measurements of the receptor-binding properties of haemagglutinin (HA) from the transmissible mutant indicate a small increase in affinity for human receptor and a marked decrease in affinity for avian receptor. From analysis of virus and HA binding data we have derived an algorithm that predicts virus avidity from the affinity of individual HA-receptor interactions. It reveals that the transmissible-mutant virus has a 200-fold preference for binding human over avian receptors. The crystal structure of the transmissible-mutant HA in complex with receptor analogues shows that it has acquired the ability to bind human receptor in the same folded-back conformation as seen for HA from the 1918, 1957 (ref. 4), 1968 (ref. 5) and 2009 (ref. 6) pandemic viruses. This binding mode is substantially different from that by which non-transmissible wild-type H5 virus HA binds human receptor. The structure of the complex also explains how the change in preference from avian to human receptors arises from the Gln226Leu substitution, which facilitates binding to human receptor but restricts binding to avian receptor. Both features probably contribute to the acquisition of transmissibility by this mutant virus.

Host Specificity Animals Birds Chick Embryo Crystallography, X-Ray Ferrets Hemagglutinin Glycoproteins, Influenza Virus Humans Influenza A Virus, H5N1 Subtype Models, Biological Models, Molecular Mutation Orthomyxoviridae Infections Protein Conformation Receptors, Virus Species Specificity

Structured evidence records

Evidence records

4 total

Genomic Evolution 1 records

Genomic Evolution Extraction confidence 0.90

Key finding

Structural analysis of a ferret-transmissible H5N1 mutant revealed that a Gln226Leu change in HA enabled a human-like receptor binding conformation resembling pandemic strains.

Virus

Host

Location

Supporting text

The crystal structure of the transmissible-mutant HA in complex with receptor analogues shows that it has acquired the ability to bind human receptor in the same folded-back conformation as seen for HA from the 1918, 1957, 1968 and 2009 pandemic viruses.

Genes or proteins: hemagglutinin (HA)
Analysis methods: crystal structure analysis; comparative structural analysis

Host Range Experiment 1 records

Host Range Experiment Extraction confidence 0.80

Key finding

The ferret-transmissible H5N1 mutant showed experimentally measured receptor-binding preference for human receptors over avian receptors, demonstrating altered host specificity underlying its transmissibility in ferrets.

Virus

Host

Location

Supporting text

Quantitative biophysical measurements of the receptor-binding properties of haemagglutinin (HA) from the transmissible mutant indicate a small increase in affinity for human receptor and a marked decrease in affinity for avian receptor. The transmissible-mutant virus has a 200-fold preference for binding human over avian receptors.

Method: quantitative biophysical measurement; receptor-binding assay; crystal structure analysis
Experimental system: in vitro cell receptor-binding assay

Molecular Adaptation 1 records

Molecular Adaptation Extraction confidence 0.95

Key finding

The Gln226Leu mutation in HA of a ferret-transmissible H5N1 virus increases binding to human receptors and decreases binding to avian receptors, contributing to host adaptation and transmissibility.

Virus

Host

Location

Supporting text

The structure of the complex also explains how the change in preference from avian to human receptors arises from the Gln226Leu substitution, which facilitates binding to human receptor but restricts binding to avian receptor.

Genes or proteins: HA
Receptors: human receptor; avian receptor
Mutations: Gln226Leu
Mechanism types: receptor_binding; host_range_shift; transmission_fitness

Receptor Usage 1 records

Receptor Usage Extraction confidence 1.00

Key finding

A ferret-transmissible H5N1 mutant exhibits greatly increased affinity for human-type receptors and decreased affinity for avian-type receptors due to the HA Gln226Leu substitution.

Virus

Host

Location

Supporting text

Quantitative biophysical measurements of the receptor-binding properties of haemagglutinin (HA) from the transmissible mutant indicate a small increase in affinity for human receptor and a marked decrease in affinity for avian receptor. The Gln226Leu substitution facilitates binding to human receptor but restricts binding to avian receptor.

Method: biophysical measurement; crystal structure analysis
Receptors: human receptor

Citation context

References

30 references

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Evidence overview

Evidence 4

Types 4

Virus 1

Host 3

Evidence types

Genomic Evolution 1 Host Range Experiment 1 Molecular Adaptation 1 Receptor Usage 1

Linked entities

Viruses

Hosts

Locations

Publication metadata

Journal: Nature
Volume / Issue / Pages: 497 / 7449 / 392-6
ISSN: 1476-4687
Journal country: England
DOI: 10.1038/nature12144