Literature detail

A Single Amino Acid Substitution at Residue 218 of Hemagglutinin Improves the Growth of Influenza A(H7N9) Candidate Vaccine Viruses.

Xing Li¹ Yamei Gao² Zhiping Ye¹

Affiliations 2 institutions

Division of Viral Products, Center for Biologics Evaluation and Research, Silver Spring, Maryland, USA [email protected] [email protected].
Division of Viral Products, Center for Biologics Evaluation and Research, Silver Spring, Maryland, USA.

PMID 31270231 2019 J Virol eng epublish

Article

Publication summary

The potential avian influenza pandemic remains a threat to public health, as the avian-origin influenza A(H7N9) virus has caused more than 1,560 laboratory-confirmed human infections since 2013, with nearly 40% mortality. Development of low-pathogenic candidate vaccine viruses (CVVs) for vaccine production is essential for pandemic preparedness. However, the suboptimal growth of CVVs in mammalian cells and chicken eggs is often a challenge. By introducing a single adaptive substitution, G218E, into the hemagglutinin (HA), we generated reassortant A(H7N9)-G218E CVVs that were characterized by significantly enhanced growth in both cells and eggs. These G218E CVVs retained the original antigenicity, as determined by a hemagglutination inhibition assay, and effectively protected ferrets from lethal challenge with the highly pathogenic parental virus. We found that the suboptimal replication of the parental H7 CVVs was associated with impeded progeny virus release as a result of strong HA receptor binding relative to weak neuraminidase (NA) cleavage of receptors. In contrast, the G218E-mediated growth improvement was attributed to relatively balanced HA and NA functions, resulted from reduced HA binding to both human- and avian-type receptors, and thus facilitated NA-mediated virus release. Our findings revealed that a single amino acid mutation at residue 218 of the HA improved the growth of A(H7N9) influenza virus by balancing HA and NA functions, shedding light on an alternative approach for optimizing certain influenza CVVs.IMPORTANCE The circulating avian influenza A(H7N9) has caused recurrent epidemic waves with high mortality in China since 2013, in which the alarming fifth wave crossing 2016 and 2017 was highlighted by a large number of human infections and the emergence of highly pathogenic avian influenza (HPAI) A(H7N9) strains in human cases. We generated low-pathogenic reassortant CVVs derived from the emerging A(H7N9) with improved virus replication and protein yield in both MDCK cells and eggs by introducing a single substitution, G218E, into HA, which was associated with reducing HA receptor binding and subsequently balancing HA-NA functions. The in vitro and in vivo experiments demonstrated comparable antigenicity of the G218E CVVs with that of their wild-type (WT) counterparts, and both the WT and the G218E CVVs fully protected ferrets from parental HPAI virus challenge. With high yield traits and the anticipated antigenicity, the G218E CVVs should benefit preparedness against the threat of an A(H7N9) influenza pandemic.

balancing HA and NA functions influenza A(H7N9) virus pandemic preparedness pathogenesis in ferret vaccine protein yield virus replication Amino Acid Substitution Adaptation, Biological Animals Chick Embryo Disease Models, Animal Dogs Ferrets Hemagglutinin Glycoproteins, Influenza Virus Influenza A Virus, H7N9 Subtype Influenza Vaccines Madin Darby Canine Kidney Cells Mutant Proteins

Structured evidence records

Evidence records

4 total

Host Range Experiment 1 records

Host Range Experiment Extraction confidence 0.90

Key finding

The G218E mutation in the HA of influenza A(H7N9) increased viral replication in MDCK cells and chicken eggs and conferred full protection in ferrets against challenge with the parental highly pathogenic virus.

Virus

Host

Location

Supporting text

By introducing a single adaptive substitution, G218E, into the hemagglutinin (HA), we generated reassortant A(H7N9)-G218E CVVs that were characterized by significantly enhanced growth in both cells and eggs. These G218E CVVs retained the original antigenicity and effectively protected ferrets from lethal challenge with the highly pathogenic parental virus.

Method: experimental infection; virus replication assay; challenge study
Sample type: MDCK cells; chicken eggs
Experimental system: in vitro and in vivo

Molecular Adaptation 1 records

Molecular Adaptation Extraction confidence 0.95

Key finding

The G218E substitution in HA of influenza A(H7N9) reduces receptor binding and balances HA and NA functions, leading to enhanced replication efficiency in mammalian cells and eggs.

Virus

Host

Location

Supporting text

By introducing a single adaptive substitution, G218E, into the hemagglutinin (HA), we generated reassortant A(H7N9)-G218E CVVs that were characterized by significantly enhanced growth in both cells and eggs. The G218E-mediated growth improvement was attributed to relatively balanced HA and NA functions, resulted from reduced HA binding to both human- and avian-type receptors.

Genes or proteins: HA; NA
Receptors: human-type receptors; avian-type receptors
Mutations: G218E
Mechanism types: receptor_binding; replication_efficiency; polymerase_activity; virus_release

Receptor Usage 1 records

Receptor Usage Extraction confidence 0.90

Key finding

Mutation G218E in influenza A(H7N9) hemagglutinin reduced binding affinity to human- and avian-type receptors, balancing HA and NA activities and improving viral replication.

Virus

Host

Location

Supporting text

The G218E-mediated growth improvement was attributed to relatively balanced HA and NA functions, resulted from reduced HA binding to both human- and avian-type receptors, and thus facilitated NA-mediated virus release.

Receptors: human- and avian-type receptors

Recombination Or Reassortment 1 records

Recombination Or Reassortment Extraction confidence 0.75

Key finding

Reassortant A(H7N9)-G218E candidate vaccine viruses were produced and showed improved replication in mammalian cells and eggs compared with parental strains.

Virus

Host

Location

Supporting text

Event type: reassortment
Genes or segments: HA

Citation context

References

47 references

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PMID 28583578	2017. Epidemiology of avian influenza A H7N9 virus in human beings across five epidemics in mainland China, 2013-17: an epidemiological study of laboratory-confirmed case series	Wang	2013
PMID 30553653 In OmniVira	Highly Pathogenic Avian H7N9 Influenza Viruses: Recent Challenges.	Ma	2019
PMID 29070694	2018. Emergence and adaptation of a novel highly pathogenic H7N9 influenza virus in birds and humans from a 2013 human-infecting low-pathogenic ancestor	Qi	2013
PMID 29056430 In OmniVira	A Highly Pathogenic Avian H7N9 Influenza Virus Isolated from A Human Is Lethal in Some Ferrets Infected via Respiratory Droplets.	Imai	2017
PMID 30305359	2018. Risk assessment of fifth-wave H7N9 influenza A viruses in mammalian models	Sun	2018
PMID 24719414	2014. Development of a high-yield live attenuated H7N9 influenza virus vaccine that provides protection against homologous and heterologous H7 wild-type viruses in ferrets	Chen	2014
PMID 25962412	2015. Development of influenza A(H7N9) candidate vaccine viruses with improved hemagglutinin antigen yield in eggs. Influenza Other Respir Viruses 9:263–270	Ridenour	2015
PMID 28162820	2017. Manipulation of neuraminidase packaging signals and hemagglutinin residues improves the growth of A/Anhui/1/2013 (H7N9) influenza vaccine virus yield in eggs. Vaccine 35:1424–1430	Barman	2017
PMID 26657023	2016. Development of a high-yield reassortant influenza vaccine virus derived from the A/Anhui/1/2013 (H7N9) strain. Vaccine 34:328–333	Nakamura	2015
PMID 26405798	2015. Generation and characterization of live attenuated influenza A(H7N9) candidate vaccine virus based on Russian donor of attenuation	Shcherbik	2015
PMID 23698299	2013. Induction of cross-reactive antibodies to novel H7N9 influenza virus by recombinant Newcastle disease virus expressing a North American lineage H7 subtype hemagglutinin	Goff	2013
PMID 29982588	2019. Antigenic drift of influenza A(H7N9) virus hemagglutinin	Ning	2019
PMID 23965618	2013. R292K substitution and drug susceptibility of influenza A(H7N9) viruses	Sleeman	2013
PMID 24696487	2014. Airborne transmission of highly pathogenic H7N1 influenza virus in ferrets	Sutton	2014
PMID 23746830 In OmniVira	Glycan receptor binding of the influenza A virus H7N9 hemagglutinin.	Tharakaraman	2013
PMID 12627392	2003. Natural and synthetic sialic acid-containing inhibitors of influenza virus receptor binding. Rev Med Virol 13:85–97	Matrosovich	2003
PMID 3608984	1987. The receptor-binding and membrane-fusion properties of influenza virus variants selected using anti-haemagglutinin monoclonal antibodies. EMBO J 6:1459–1465	Daniels	1987
PMID 25673693	2015. Avian influenza virus infection of immortalized human respiratory epithelial cells depends upon a delicate balance between hemagglutinin acid stability and endosomal pH	Daidoji	2015
PMID 22085243	2012. Influenza neuraminidase. Influenza Other Respir Viruses 6:245–256	Air	2011
PMID 20538598	2010. Influenza hemagglutinin and neuraminidase membrane glycoproteins	Gamblin	2010
PMID 22013054	2012. Amino acid changes in hemagglutinin contribute to the replication of oseltamivir-resistant H1N1 influenza viruses	Ginting	2012
PMID 10846083	2000. Balanced hemagglutinin and neuraminidase activities are critical for efficient replication of influenza A virus	Mitnaul	2000
PMID 22718832 In OmniVira	Functional balance of the hemagglutinin and neuraminidase activities accompanies the emergence of the 2009 H1N1 influenza pandemic.	Xu	2012
PMID 22379077	2012. Decreased neuraminidase activity is important for the adaptation of H5N1 influenza virus to human airway epithelium	Ilyushina	2012
PMID 23408613	2013. Identification of critical residues in the hemagglutinin and neuraminidase of influenza virus H1N1pdm for vaccine virus replication in embryonated chicken eggs	Wang	2013
PMID 6191220	1983. Single amino acid substitutions in influenza haemagglutinin change receptor binding specificity	Rogers	1983
PMID 23842497 In OmniVira	Pathogenesis and transmission of avian influenza A (H7N9) virus in ferrets and mice.	Belser	2013
PMID 24162312 In OmniVira	Adaptation of novel H7N9 influenza A virus to human receptors.	Dortmans	2013
PMID 23842494	2013. Characterization of H7N9 influenza A viruses isolated from humans	Watanabe	2013
PMID 26792744 In OmniVira	Amino Acid Substitutions That Affect Receptor Binding and Stability of the Hemagglutinin of Influenza A/H7N9 Virus.	Schrauwen	2016
PMID 24009358 In OmniVira	Structures and receptor binding of hemagglutinins from human-infecting H7N9 influenza viruses.	Shi	2013
PMID 23823727	2013. Biological features of novel avian influenza A (H7N9) virus	Zhou	2013
PMID 25850788 In OmniVira	Mammalian adaptation of influenza A(H7N9) virus is limited by a narrow genetic bottleneck.	Zaraket	2015
PMID 23787694 In OmniVira	Receptor binding by an H7N9 influenza virus from humans.	Xiong	2013
PMID 23950563 In OmniVira	H7N9 influenza viruses interact preferentially with α2,3-linked sialic acids and bind weakly to α2,6-linked sialic acids.	Ramos	2013
PMID 9060710	1997. Differences in sialic acid-galactose linkages in the chicken egg amnion and allantois influence human influenza virus receptor specificity and variant selection	Ito	1997
PMID 24058646	2013. Heterogeneity of the MDCK cell line and its applicability for influenza virus research	Lugovtsev	2013
PMID 24161712	2014. Receptor binding and pH stability: how influenza A virus hemagglutinin affects host-specific virus infection. Biochim Biophys Acta 1838:1153–1168	Mair	2013
PMID 9342319	1997. Structural evidence for a second sialic acid binding site in avian influenza virus neuraminidases	Varghese	1997
PMID 6485252	1984. Influenza virus neuraminidase with hemagglutinin activity. Virology 137:323	Laver	1984
PMID 28356530 In OmniVira	Role of Neuraminidase in Influenza A(H7N9) Virus Receptor Binding.	Benton	2017
PMID 28202753 In OmniVira	Mutation of the Second Sialic Acid-Binding Site, Resulting in Reduced Neuraminidase Activity, Preceded the Emergence of H7N9 Influenza A Virus.	Dai	2017
PMID 23577628	2013. Human infection with a novel avian-origin influenza A (H7N9) virus	Gao	2013
PMID 10801978	2000. A DNA transfection system for generation of influenza A virus from eight plasmids	Hoffmann	2000
PMID 22528152	2012. Influenza virus titration, antigenic characterization, and serological methods for antibody detection. Methods Mol Biol 865:25–51	Klimov	2012
PMID 6260835	1980. Microneutralization test for influenza A and B and parainfluenza 1 and 2 viruses that uses continuous cell lines and fresh serum enhancement	Frank	1980
PMID 19224999	2009. Optimizing viral protein yield of influenza virus strain A/Vietnam/1203/2004 by modification of the neuraminidase gene	Adamo	2004

Evidence overview

Evidence 4

Types 4

Virus 1

Host 3

Evidence types

Host Range Experiment 1 Molecular Adaptation 1 Receptor Usage 1 Recombination Or Reassortment 1

Linked entities

Viruses

Hosts

Locations

Publication metadata

Journal: Journal of virology
Volume / Issue / Pages: 93 / 19 / -
ISSN: 1098-5514
Journal country: United States
DOI: 10.1128/JVI.00570-19