Literature detail

Molecular Characterizations of Surface Proteins Hemagglutinin and Neuraminidase from Recent H5Nx Avian Influenza Viruses.

Hua Yang¹ Paul J Carney¹ Vasiliy P Mishin¹ Zhu Guo¹ Jessie C Chang¹ David E Wentworth¹ Larisa V Gubareva¹ James Stevens²

Affiliations 2 institutions

Influenza Division, National Center for Immunization and Respiratory Diseases, Centers for Disease Control and Prevention, Atlanta, Georgia, USA.
Influenza Division, National Center for Immunization and Respiratory Diseases, Centers for Disease Control and Prevention, Atlanta, Georgia, USA [email protected].

PMID 27053557 2016 J Virol eng epublish

PubMed DOI Browse context

Article

Publication summary

During 2014, a subclade 2.3.4.4 highly pathogenic avian influenza (HPAI) A(H5N8) virus caused poultry outbreaks around the world. In late 2014/early 2015, the virus was detected in wild birds in Canada and the United States, and these viruses also gave rise to reassortant progeny, composed of viral RNA segments (vRNAs) from both Eurasian and North American lineages. In particular, viruses were found with N1, N2, and N8 neuraminidase vRNAs, and these are collectively referred to as H5Nx viruses. In the United States, more than 48 million domestic birds have been affected. Here we present a detailed structural and biochemical analysis of the surface antigens of H5N1, H5N2, and H5N8 viruses in addition to those of a recent human H5N6 virus. Our results with recombinant hemagglutinin reveal that these viruses have a strict avian receptor binding preference, while recombinantly expressed neuraminidases are sensitive to FDA-approved and investigational antivirals. Although H5Nx viruses currently pose a low risk to humans, it is important to maintain surveillance of these circulating viruses and to continually assess future changes that may increase their pandemic potential. The H5Nx viruses emerging in North America, Europe, and Asia pose a great public health concern. Here we report a molecular and structural study of the major surface proteins of several H5Nx influenza viruses. Our results improve the understanding of these new viruses and provide important information on their receptor preferences and susceptibilities to antivirals, which are central to pandemic risk assessment.

Animals Animals, Wild Asia Canada Disease Outbreaks Europe Hemagglutinin Glycoproteins, Influenza Virus Humans Influenza A Virus, H5N1 Subtype Influenza A Virus, H5N2 Subtype Influenza A Virus, H5N8 Subtype Influenza in Birds Influenza, Human Neuraminidase North America Phylogeny Poultry Reassortant Viruses

Structured evidence records

Evidence records

5 total

Zoonotic Surveillance 2 records

Zoonotic Surveillance Extraction confidence 0.60

Key finding

H5Nx avian influenza viruses were detected in wild birds in Canada and the United States during 2014–2015 as part of surveillance reporting of these emerging strains.

Virus

Host

Location

Supporting text

In late 2014/early 2015, the virus was detected in wild birds in Canada and the United States, and these viruses also gave rise to reassortant progeny.

Geographic raw: Canada
Country inferred: Canada

Zoonotic Surveillance Extraction confidence 0.60

Key finding

H5Nx avian influenza viruses were detected in wild birds in the United States during 2014–2015, indicating active monitoring of these avian populations.

Virus

Host

Location

Supporting text

In late 2014/early 2015, the virus was detected in wild birds in Canada and the United States, and these viruses also gave rise to reassortant progeny.

Geographic raw: United States
Country inferred: United States

Genomic Evolution 1 records

Genomic Evolution Extraction confidence 0.70

Key finding

H5Nx avian influenza viruses in North America arose through reassortment of Eurasian and North American RNA segment lineages, with genetic and phylogenetic characterization of their hemagglutinin and neuraminidase genes.

Virus

Host

Location

Supporting text

During 2014, a subclade 2.3.4.4 highly pathogenic avian influenza (HPAI) A(H5N8) virus caused poultry outbreaks around the world. ... the virus was detected in wild birds in Canada and the United States, and these viruses also gave rise to reassortant progeny, composed of viral RNA segments (vRNAs) from both Eurasian and North American lineages. In particular, viruses were found with N1, N2, and N8 neuraminidase vRNAs, and these are collectively referred to as H5Nx viruses. ... Here we present a detailed structural and biochemical analysis of the surface antigens of H5N1, H5N2, and H5N8 viruses ... MeSH terms include 'Hemagglutinin Glycoproteins, Influenza Virus / genetics', 'Neuraminidase / genetics', and 'Phylogeny'.

Genes or proteins: hemagglutinin; neuraminidase
Analysis methods: genetic characterization; phylogenetic analysis

Receptor Usage 1 records

Receptor Usage Extraction confidence 0.95

Key finding

Recombinant hemagglutinin of H5Nx highly pathogenic avian influenza viruses shows strict binding to avian-type receptors.

Virus

Host

Location

Supporting text

Our results with recombinant hemagglutinin reveal that these viruses have a strict avian receptor binding preference.

Method: structural analysis; biochemical analysis
Receptors: avian receptor

Recombination Or Reassortment 1 records

Recombination Or Reassortment Extraction confidence 0.90

Key finding

H5Nx avian influenza viruses emerged as reassortants combining viral RNA segments from Eurasian and North American lineages.

Virus

Host

Location

Supporting text

These viruses also gave rise to reassortant progeny, composed of viral RNA segments (vRNAs) from both Eurasian and North American lineages.

Event type: reassortment
Genes or segments: viral RNA segments

Citation context

References

75 references

Reference network

Force-directed citation graph. OmniVira-indexed references are prioritized and recursively expanded up to three steps.

260 nodes · 529 links · capped

Drag nodes to explore citation neighborhoods


PMID 9482437	1998. Clinical features and rapid viral diagnosis of human disease associated with avian influenza A H5N1 virus	Yuen	1998
-	17 July 2015	WHO. 17 July	2015
PMID 18818732 In OmniVira	Evolutionary dynamics and emergence of panzootic H5N1 influenza viruses.	Vijaykrishna	2008
PMID 25966311	2015	Smith	2014
PMID 26143617	2015. Human infection with a novel highly pathogenic avian influenza A (H5N6) virus: virological and clinical findings	Pan	2015
-	2014	World Organisation for Animal Health	2014
PMID 25898265	2015. Novel Eurasian highly pathogenic avian influenza A H5 viruses in wild birds, Washington, USA, 2014	Ip	2014
PMID 1579108	1992. Evolution and ecology of influenza A viruses. Microbiol Rev 56:152–179	Webster	1992
PMID 9201232	1997. Avian influenza A viruses differ from human viruses by recognition of sialyloligosaccharides and gangliosides and by a higher conservation of the HA receptor-binding site. Virology 233:224–234	Matrosovich	1997
PMID 6191220	1983. Single amino acid substitutions in influenza haemagglutinin change receptor binding specificity	Rogers	1983
PMID 7815489	1995. Influenza type A virus neuraminidase does not play a role in viral entry, replication, assembly, or budding	Liu	1995
PMID 16192481	2005. Neuraminidase inhibitors for influenza	Moscona	2005
PMID 14764887	2004. Structure of the uncleaved human H1 hemagglutinin from the extinct 1918 influenza virus	Stevens	1918
PMID 15569942	2004. The VASP tetramerization domain is a right-handed coiled coil based on a 15-residue repeat	Kuhnel	2004
PMID 18715929	2008. Structural characterization of the 1918 influenza H1N1 neuraminidase	Xu	1918
PMID 17272842	2007. Optimization techniques for automation and high throughput. Methods Mol Biol 363:175–190	Chayen	2007
PMID 27754618	1997. Processing of X-ray diffraction data collected in oscillation mode. Methods Enzymol 276:307–326	Otwinowski	1997
PMID 15805601	2005. Likelihood-enhanced fast translation functions. Acta Crystallogr D Biol Crystallogr 61:458–464	McCoy	2005
PMID 24086467 In OmniVira	Structural and antigenic variation among diverse clade 2 H5N1 viruses.	Shore	2013
PMID 15572765	2004. Coot: model-building tools for molecular graphics. Acta Crystallogr D Biol Crystallogr 60:2126–2132	Emsley	2004
PMID 15299374	1994	CCP4	1994
PMID 11134934	2001. Use of TLS parameters to model anisotropic displacements in macromolecular refinement. Acta Crystallogr D Biol Crystallogr 57:122–133	Winn	2001
PMID 20124702	2010. PHENIX: a comprehensive Python-based system for macromolecular structure solution. Acta Crystallogr D Biol Crystallogr 66:213–221	Adams	2010
PMID 22028647	2011. Structural and functional analysis of laninamivir and its octanoate prodrug reveals group specific mechanisms for influenza NA inhibition	Vavricka	2011
PMID 24899180	2014. Structure of influenza virus N7: the last piece of the neuraminidase “jigsaw” puzzle	Sun	2014
PMID 25540377 In OmniVira	Structural and functional analysis of surface proteins from an A(H3N8) influenza virus isolated from New England harbor seals.	Yang	2015
PMID 17452350	2007. MolProbity: all-atom contacts and structure validation for proteins and nucleic acids	Davis	2007
PMID 16343533 In OmniVira	Glycan microarray analysis of the hemagglutinins from modern and pandemic influenza viruses reveals different receptor specificities.	Stevens	2006
PMID 16543414 In OmniVira	Structure and receptor specificity of the hemagglutinin from an H5N1 influenza virus.	Stevens	2006
PMID 20352039	2010. Structure and receptor binding properties of a pandemic H1N1 virus hemagglutinin	Yang	2010
PMID 22674977	2012. Structure and receptor complexes of the hemagglutinin from a highly pathogenic H7N7 influenza virus	Yang	2012
PMID 20824086 In OmniVira	Structures of receptor complexes of a North American H7N2 influenza hemagglutinin with a loop deletion in the receptor binding site.	Yang	2010
PMID 464297	1979. Fluorometric assay of neuraminidase with a sodium (4-methylumbelliferyl-α-d- N -acetylneuraminate) substrate. Anal Biochem 94:287–296	Potier	1979
PMID 8162439	1994. Host cell proteases controlling virus pathogenicity. Trends Microbiol 2:39–43	Klenk	1994
PMID 16030144	2005. Role of domestic ducks in the propagation and biological evolution of highly pathogenic H5N1 influenza viruses in Asia	Hulse-Post	2005
PMID 11562490	2001. X-ray structures of H5 avian and H9 swine influenza virus hemagglutinins bound to avian and human receptor analogs	Ha	2001
PMID 12758169	2003. X-ray structure of the hemagglutinin of a potential H3 avian progenitor of the 1968 Hong Kong pandemic influenza virus. Virology 309:209–218	Ha	1968
PMID 19805083	2009. Structures of receptor complexes formed by hemagglutinins from the Asian influenza pandemic of 1957	Liu	1957
PMID 15246268	2004. H1 and H7 influenza haemagglutinin structures extend a structural classification of haemagglutinin subtypes. Virology 325:287–296	Russell	2004
PMID 19004788	2008. Structure of influenza hemagglutinin in complex with an inhibitor of membrane fusion	Russell	2008
PMID 7464906	1981. Structure of the haemagglutinin membrane glycoprotein of influenza virus at 3 Å resolution	Wilson	1981
PMID 23760233	2013. Structure and receptor binding specificity of hemagglutinin H13 from avian influenza A virus H13N6	Lu	2013
PMID 22993148	2012. Insights into avian influenza virus pathogenicity: the hemagglutinin precursor HA0 of subtype H16 has an α-helix structure in its cleavage site with inefficient HA1/HA2 cleavage	Lu	2012
PMID 14764886	2004. The structure and receptor binding properties of the 1918 influenza hemagglutinin	Gamblin	1918
PMID 9814710	1998. Structure of the hemagglutinin precursor cleavage site, a determinant of influenza pathogenicity and the origin of the labile conformation	Chen	1998
PMID 8626433	1996. The amino acid at the X position of an Asn-X-Ser sequon is an important determinant of N-linked core-glycosylation efficiency	Shakin-Eshleman	1996
PMID 11779386	2001. The predicted antigenicity of the haemagglutinin of the 1918 Spanish influenza pandemic suggests an avian origin. Philos Trans R Soc Lond B Biol Sci 356:1871–1876	Brownlee	2001
PMID 6162101	1981. Structural identification of the antibody-binding sites of Hong Kong influenza haemagglutinin and their involvement in antigenic variation	Wiley	1981
PMID 23933511	2013. The antigenic architecture of the hemagglutinin of influenza H5N1 viruses. Mol Immunol 56:705–719	Velkov	2013
PMID 25796641	2015	Anonymous	2015
PMID 16707041	2006. Host range restriction and pathogenicity in the context of influenza pandemic	Neumann	2006
PMID 7975212	1994. Receptor specificity in human, avian, and equine H2 and H3 influenza virus isolates. Virology 205:17–23	Connor	1994
PMID 10954551	2000. Early alterations of the receptor-binding properties of H1, H2, and H3 avian influenza virus hemagglutinins after their introduction into mammals	Matrosovich	2000
PMID 22723414	2012. The potential for respiratory droplet-transmissible A/H5N1 influenza virus to evolve in a mammalian host	Russell	2012
PMID 17690300 In OmniVira	Immunization by avian H5 influenza hemagglutinin mutants with altered receptor binding specificity.	Yang	2007
PMID 20427525 In OmniVira	Glycosylation at 158N of the hemagglutinin protein and receptor binding specificity synergistically affect the antigenicity and immunogenicity of a live attenuated H5N1 A/Vietnam/1203/2004 vaccine virus in ferrets.	Wang	2010
PMID 17108965 In OmniVira	Haemagglutinin mutations responsible for the binding of H5N1 influenza A viruses to human-type receptors.	Yamada	2006
PMID 22056389	2012. In vitro evolution of H5N1 avian influenza virus toward human-type receptor specificity. Virology 422:105–113	Chen	2011
PMID 24027325 In OmniVira	Structural analysis of the hemagglutinin from the recent 2013 H7N9 influenza virus.	Yang	2013
-	15 June 2015	USDA Animal and Plant Health Inspection	2015
PMID 6843658	1983. Structure of the influenza virus glycoprotein antigen neuraminidase at 2.9 Å resolution	Varghese	1983
PMID 3447170	1987. Three-dimensional structure of neuraminidase of subtype N9 from an avian influenza virus. Proteins 2:111–117	Baker	1987
PMID 16915235	2006. The structure of H5N1 avian influenza neuraminidase suggests new opportunities for drug design	Russell	2006
PMID 21653672	2011. Influenza A virus N5 neuraminidase has an extended 150-cavity	Wang	2011
PMID 1740114	1992. The 2.2 Å resolution crystal structure of influenza B neuraminidase and its complex with sialic acid. EMBO J 11:49–56	Burmeister	1992
PMID 23824808	2013. Functional and structural analysis of influenza virus neuraminidase N3 offers further insight into the mechanisms of oseltamivir resistance	Li	2013
PMID 23012478	2012. Crystal structures of two subtype N10 neuraminidase-like proteins from bat influenza A viruses reveal a diverged putative active site	Zhu	2012
PMID 24130481	2013. New world bats harbor diverse influenza A viruses	Tong	2013
PMID 22085243	2012. Influenza neuraminidase. Influenza Other Respir Viruses 6:245–256	Air	2011
PMID 2482974	1989. The neuraminidase of influenza virus. Proteins 6:341–356	Air	1989
PMID 1628657	1992	Chong	1992
PMID 8113759	1994. Calcium is needed for the thermostability of influenza B virus neuraminidase	Burmeister	1994
PMID 16929094	2006. Structure of a calcium-deficient form of influenza virus neuraminidase: implications for substrate binding. Acta Crystallogr D Biol Crystallogr 62:947–952	Smith	2006
PMID 8031750	1994. Structure of influenza virus neuraminidase B/Lee/40 complexed with sialic acid and a dehydro analog at 1.8-Å resolution: implications for the catalytic mechanism. Biochemistry 33:8172–8179	Janakiraman	1994
-	2002. The PyMOL Molecular Graphics System. DeLano Scientific, Palo Alto, CA: www.pymol.org	DeLano	2002

Evidence overview

Evidence 5

Types 4

Virus 2

Host 1

Evidence types

Zoonotic Surveillance 2 Genomic Evolution 1 Receptor Usage 1 Recombination Or Reassortment 1

Linked entities

Viruses

Hosts

Locations

Publication metadata

Journal: Journal of virology
Volume / Issue / Pages: 90 / 12 / 5770-5784
ISSN: 1098-5514
Journal country: United States
DOI: 10.1128/JVI.00180-16