Literature detail

Changes in H5N1 influenza virus hemagglutinin receptor binding domain affect systemic spread.

Hui-Ling Yen¹ Jerry R Aldridge Adrianus C M Boon Natalia A Ilyushina Rachelle Salomon Diane J Hulse-Post Henju Marjuki John Franks David A Boltz Dorothy Bush Aleksandr S Lipatov Richard J Webby Jerold E Rehg Robert G Webster

Affiliations 1 institutions

Division of Virology, Department of Infectious Diseases, St. Jude Children's Research Hospital, Memphis, TN 38105, USA.

PMID 19116267 2009 Proc Natl Acad Sci U S A eng ppublish

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Article

Publication summary

The HA of influenza virus is a receptor-binding and fusion protein that is required to initiate infection. The HA receptor-binding domain determines the species of sialyl receptors recognized by influenza viruses. Here, we demonstrate that changes in the HA receptor-binding domain alter the ability of the H5N1 virus to spread systemically in mice. The A/Vietnam/1203/04 (VN1203) and A/Hong Kong/213/03 (HK213) viruses are consistently lethal to domestic chickens but differ in their pathogenicity to mammals. Insertion of the VN1203 HA and neuraminidase (NA) genes into recombinant HK213 virus expanded its tissue tropism and increased its lethality in mice; conversely, insertion of HK213 HA and NA genes into recombinant VN1203 virus decreased its systemic spread and lethality. The VN1203 and HK213 HAs differ by 10 aa, and HK213 HA has shown greater binding affinity for synthetic alpha2,6-linked sialyl receptor. Introduction of an S227N change and removal of N-linked glycosylation at residue 158 increased the alpha2,6-binding affinity of VN1203 HA. Recombinant VN1203 virus carrying the S227N change alone or with the residue-158 glycosylation site removed showed reduced lethality and systemic spread in mice but not in domestic chickens. Wild-type VN1203 virus exhibited the greatest efficiency in systemic spread after intramuscular inoculation and in infection of mouse bone marrow-derived dendritic cells and conventional pulmonary dendritic cells. These results show that VN1203 HA glycoprotein confers pathogenicity by facilitating systemic spread in mice; they also suggest that a minor change in receptor binding domain may modulate the virulence of H5N1 viruses.

Animals Chickens Dendritic Cells Glycosylation Hemagglutinin Glycoproteins, Influenza Virus Influenza A Virus, H5N1 Subtype Mice Mutation Neuraminidase Organisms, Genetically Modified Protein Interaction Domains and Motifs Receptors, Virus Virulence hemagglutinin, avian influenza A virus

Structured evidence records

Evidence records

4 total

Host Range Experiment 2 records

Host Range Experiment Extraction confidence 0.95

Key finding

Recombinant H5N1 viruses with VN1203 HA and NA displayed expanded tissue tropism and higher lethality in mice, indicating experimentally tested differences in host susceptibility and systemic spread.

Virus

Host

Location

Supporting text

Insertion of the VN1203 HA and neuraminidase (NA) genes into recombinant HK213 virus expanded its tissue tropism and increased its lethality in mice; conversely, insertion of HK213 HA and NA genes into recombinant VN1203 virus decreased its systemic spread and lethality. Recombinant VN1203 virus carrying the S227N change alone or with the residue-158 glycosylation site removed showed reduced lethality and systemic spread in mice but not in domestic chickens.

Method: recombinant virus infection; mutation analysis; experimental infection
Sample type: bone marrow-derived dendritic cells; pulmonary dendritic cells
Experimental system: in vivo animal experiment

Host Range Experiment Extraction confidence 0.95

Key finding

Mutant VN1203 H5N1 viruses with S227N or glycosylation removal maintained pathogenicity in domestic chickens but lost systemic spread and lethality in mice, showing host-dependent effects of HA receptor binding changes.

Virus

Host

Location

Supporting text

Recombinant VN1203 virus carrying the S227N change alone or with the residue-158 glycosylation site removed showed reduced lethality and systemic spread in mice but not in domestic chickens.

Method: recombinant virus infection; experimental infection
Experimental system: in vivo animal experiment

Molecular Adaptation 1 records

Molecular Adaptation Extraction confidence 1.00

Key finding

S227N substitution and loss of glycosylation at residue 158 in the H5N1 HA receptor-binding domain increased alpha2,6 sialic acid binding and altered virulence and systemic spread in mice, indicating molecular adaptation of H5N1 to mammalian hosts.

Virus

Host

Location

Supporting text

Introduction of an S227N change and removal of N-linked glycosylation at residue 158 increased the alpha2,6-binding affinity of VN1203 HA. Recombinant VN1203 virus carrying the S227N change alone or with the residue-158 glycosylation site removed showed reduced lethality and systemic spread in mice but not in domestic chickens.

Genes or proteins: HA
Receptors: alpha2,6-linked sialyl receptor
Mutations: S227N; loss of glycosylation at residue 158
Mechanism types: receptor_binding; pathogenicity; tissue_tropism

Receptor Usage 1 records

Receptor Usage Extraction confidence 1.00

Key finding

H5N1 hemagglutinin amino acid substitutions (S227N and removal of residue-158 glycosylation) enhanced binding to alpha2,6-linked sialyl receptor compared with HK213 HA.

Virus

Host

Location

Supporting text

HK213 HA has shown greater binding affinity for synthetic alpha2,6-linked sialyl receptor. Introduction of an S227N change and removal of N-linked glycosylation at residue 158 increased the alpha2,6-binding affinity of VN1203 HA.

Receptors: alpha2,6-linked sialyl receptor

Citation context

References

48 references

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Evidence overview

Evidence 4

Types 3

Virus 1

Host 2

Evidence types

Host Range Experiment 2 Molecular Adaptation 1 Receptor Usage 1

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Publication metadata

Journal: Proceedings of the National Academy of Sciences of the United States of America
Volume / Issue / Pages: 106 / 1 / 286-91
ISSN: 1091-6490
Journal country: United States
DOI: 10.1073/pnas.0811052106