Using Sequence Data To Infer the Antigenicity of Influenza Virus

Sun, Hailiang; Yang, Jialiang; Zhang, Tong; Liang, Liping; Jia, Kun; Yang, Guohua; Webby, Richard J.; Wan, Xiu‐Feng

doi:10.1128/mbio.00230-13

Cited by 94 publications

(114 citation statements)

References 45 publications

(65 reference statements)

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“…All sites are conserved in samples except for the loss of glycosylation observed at position 126 in 7 samples and another at position 45 in a single sample. All positions except 483 have been reported in previous studies (Sun et al, 2013). The study shows a gain of the glycosylation sites in the antigenic region since 2004.…”

Section: Ajidmentioning

confidence: 49%

“…All sites were seen to be conserved in the samples except for the loss of glycosylation seen at position 126 in 7 samples and another at position 45 in a single sample. All positions except 483 have been reported in previous studies (Sun et al, 2013). Among these sites residues 45,63,122,126,133,144,165 and 246 were found to occur on antigenic sites and these changes may alter the ability of antibodies to bind antigenic site and may thus contribute to the generation of escape mutants.…”

Section: Glycosylation Sitesmentioning

confidence: 92%

“…Influenza viruses can efficiently escape from host antibodies by means of accumulation of mutations in their surface glycoproteins HA and NA (antigenic drift) or by the introduction of new subtypes of these glycoproteins through gene segment reassortment (antigenic shift) and it has been observed that antigenic drift occurs more frequently in H3N2 viruses than any other seasonal virus, which is reflected by the number of times H3N2 vaccine strain has been updated in comparison to H1N1 and influenza B virus (Sun et al, 2013).…”

Section: Discussionmentioning

confidence: 99%

“…It has been suggested that amino acid changes occurring in epitopes of high neutralization efficiencies (i.e., epitope A, B and D) are associated with antigenic drift, rather than those in epitope of low neutralization efficiencies (i.e., C and E) (Sun et al, 2013;Ndifon et al, 2009). It has been also been proposed that a minimum of four substitutions in two or more antigenic sites of HA protein were required for an epidemically important strain (Huang et al, 2011).…”

Section: Discussionmentioning

confidence: 99%

“…HA1 forms the globular head domain which contains the receptor binding site for sialic acid receptor present on host cells, along with 5 antigenic sites (A-E) (Bush et al, 1999). HA1 mutates more frequently than HA2 and plays a major role in natural selection and antibody escape (Sun et al, 2013).…”

Section: Introductionmentioning

confidence: 99%

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Molecular Characterization on the Basis of Ha, Na and M Gene Revealed Changes in Critical Amino Acid Positions of Influenza a (H3n2) Virus Circulating in India During 2011-2013

Kumar¹,

Khare²,

Saidullah³

et al. 2014

American Journal of Infectious Diseases

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Influenza A (H1N1) virus is responsible for acute respiratory infection in human, which occasionally causes epidemic and rarely a pandemic. Full length DNA sequencing of HA, NA and M gene of H3N2 virus from year 2011-2013 was performed for determination of the circulating strains in India along with monitoring status of various mutations associated with drug resistance and virulence. Genetic analysis of HA gene of study samples in comparison to reference strain showed maximum amino acid changes in epitopes of high neutralization efficiencies (antigenic sites A, B and D) along with gain of glycosylation sites at position 45 (except single sample) and loss at position 126 (7 samples). NA gene has four amino acid changes in antibody binding region at position S367N, K369T, S332F and S334I along with gain and loss of glycosylation site at position 367 and 402 respectively whereas no change was observed in its active site. While comparison of deduced amino acid sequences of study samples with Indian strains from earlier years showed six amino acid changes in three antigenic sites on HA protein and three amino acid changes in NA protein epitope sequence. All these changes indicate that the H3N2 virus is undergoing antigenic drift and which may result in the emergence of new antigenic variants. We want to report that our study provided for the first time full length matrix gene sequence of influenza A (H3N2) virus from India.

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Section: Ajidmentioning

confidence: 49%

Section: Glycosylation Sitesmentioning

confidence: 92%

Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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Molecular Characterization on the Basis of Ha, Na and M Gene Revealed Changes in Critical Amino Acid Positions of Influenza a (H3n2) Virus Circulating in India During 2011-2013

Kumar¹,

Khare²,

Saidullah³

et al. 2014

American Journal of Infectious Diseases

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Antigenic characterization of influenza and SARS-CoV-2 viruses

2021

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Antigenic characterization of emerging and re-emerging viruses is necessary for the prevention of and response to outbreaks, evaluation of infection mechanisms, understanding of virus evolution, and selection of strains for vaccine development. Primary analytic methods, including enzyme-linked immunosorbent/lectin assays, hemagglutination inhibition, neuraminidase inhibition, micro-neutralization assays, and antigenic cartography, have been widely used in the field of influenza research. These techniques have been improved upon over time for increased analytical capacity, and some have been mobilized for the rapid characterization of the SARS-CoV-2 virus as well as its variants, facilitating the development of highly effective vaccines within 1 year of the initially reported outbreak. While great strides have been made for evaluating the antigenic properties of these viruses, multiple challenges prevent efficient vaccine strain selection and accurate assessment. For influenza, these barriers include the requirement for a large virus quantity to perform the assays, more than what can typically be provided by the clinical samples alone, cell- or egg-adapted mutations that can cause antigenic mismatch between the vaccine strain and circulating viruses, and up to a 6-month duration of vaccine development after vaccine strain selection, which allows viruses to continue evolving with potential for antigenic drift and, thus, antigenic mismatch between the vaccine strain and the emerging epidemic strain. SARS-CoV-2 characterization has faced similar challenges with the additional barrier of the need for facilities with high biosafety levels due to its infectious nature. In this study, we review the primary analytic methods used for antigenic characterization of influenza and SARS-CoV-2 and discuss the barriers of these methods and current developments for addressing these challenges.

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