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Divergent genetic evolution of hemagglutinin in influenza A H1N1 and A H1N2 subtypes isolated in the south-France since the winter of 2001-2002.

Identifieur interne : 000252 ( France/Analysis ); précédent : 000251; suivant : 000253

Divergent genetic evolution of hemagglutinin in influenza A H1N1 and A H1N2 subtypes isolated in the south-France since the winter of 2001-2002.

Auteurs : S. Al Faress [France] ; G. Cartet [France] ; O. Ferraris [France] ; H. Norder [France] ; M. Valette [France] ; B. Lina [France]

Source :

RBID : Hal:hal-00125068

Descripteurs français

English descriptors

Abstract

BACKGROUND: Influenza A viruses are divided into subtypes based on their hemagglutinin (H1 to H15) and neuraminidase (N1 to N9) glycoproteins. Of these, three A subtypes H1N1, H3N2 and H1N2 circulate in the human population. Influenza A viruses display a high antigenic variability called "antigenic drift" which allows the virus to escape antibody neutralization. OBJECTIVES: Evaluate the mutations apparition that might predict a divergent antigenic evolution of hemagglutinin in influenza A H1N1 and A H1N2 viruses. STUDY DESIGN: During the three winters of 2001-2002 to 2003-2004, 58 A H1N1 and 23 A H1N2 subtypes have been isolated from patients with influenza-like illness in the south of France. The HA1 region was analyzed by RT-PCR and subsequently sequenced to compare the HA1 genetic evolution of influenza A H1N1 and A H1N2 subtypes. RESULTS: Our results showed that 28 amino acid substitutions have accumulated in the HA1 region since the circulation of A/New Caledonia/20/99-like viruses in France. Of these, fifteen were located in four antigenic sites (B, C, D and E). Six of them were observed only in the A H1N2 isolates, six only in the A H1N1 isolates and three in both subtypes. Furthermore, nine of twenty two A H1N2 isolates from the winter of 2002-2003 shared a T90A amino acid change which has not been observed in any A H1N1 isolate; resulting in the introduction of a new glycosylation site close to the antigenic site E. This might mask some antigenic E determinants and therefore, modify the A H1N2 antigenicity. CONCLUSIONS: The divergent genetic evolution of hemagglutinin may ultimately lead to a significant different antigenicity between A H1N1 and A H1N2 subtypes that would require the introduction of a new subtype in the vaccine batches.


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Hal:hal-00125068

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<orgName type="acronym">VPV</orgName>
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<orgName type="acronym">UCBL</orgName>
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<addrLine>43, boulevard du 11 novembre 1918, 69622 Villeurbanne cedex</addrLine>
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<addrLine>92 rue Pasteur - CS 30122, 69361 Lyon Cedex 07</addrLine>
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<ref type="url">https://www.universite-lyon.fr/</ref>
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<region type="old region" nuts="2">Rhône-Alpes</region>
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<term>Animals</term>
<term>Cell Line</term>
<term>DNA</term>
<term>Dogs</term>
<term>Evolution</term>
<term>France</term>
<term>H1N1 Subtype</term>
<term>Hemagglutination Inhibition Tests</term>
<term>Hemagglutinin Glycoproteins</term>
<term>Human/virology</term>
<term>Humans</term>
<term>Influenza</term>
<term>Influenza A Virus</term>
<term>Influenza A virus/*classification/*genetics/isolation & purification</term>
<term>Influenza Virus/*genetics</term>
<term>Molecular</term>
<term>Phylogeny</term>
<term>Sequence Analysis</term>
</keywords>
<keywords scheme="Wicri" type="topic" xml:lang="fr">
<term>ADN</term>
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<keywords scheme="Wicri" type="geographic" xml:lang="fr">
<term>France</term>
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<div type="abstract" xml:lang="en">
<p>BACKGROUND: Influenza A viruses are divided into subtypes based on their hemagglutinin (H1 to H15) and neuraminidase (N1 to N9) glycoproteins. Of these, three A subtypes H1N1, H3N2 and H1N2 circulate in the human population. Influenza A viruses display a high antigenic variability called "antigenic drift" which allows the virus to escape antibody neutralization. OBJECTIVES: Evaluate the mutations apparition that might predict a divergent antigenic evolution of hemagglutinin in influenza A H1N1 and A H1N2 viruses. STUDY DESIGN: During the three winters of 2001-2002 to 2003-2004, 58 A H1N1 and 23 A H1N2 subtypes have been isolated from patients with influenza-like illness in the south of France. The HA1 region was analyzed by RT-PCR and subsequently sequenced to compare the HA1 genetic evolution of influenza A H1N1 and A H1N2 subtypes. RESULTS: Our results showed that 28 amino acid substitutions have accumulated in the HA1 region since the circulation of A/New Caledonia/20/99-like viruses in France. Of these, fifteen were located in four antigenic sites (B, C, D and E). Six of them were observed only in the A H1N2 isolates, six only in the A H1N1 isolates and three in both subtypes. Furthermore, nine of twenty two A H1N2 isolates from the winter of 2002-2003 shared a T90A amino acid change which has not been observed in any A H1N1 isolate; resulting in the introduction of a new glycosylation site close to the antigenic site E. This might mask some antigenic E determinants and therefore, modify the A H1N2 antigenicity. CONCLUSIONS: The divergent genetic evolution of hemagglutinin may ultimately lead to a significant different antigenicity between A H1N1 and A H1N2 subtypes that would require the introduction of a new subtype in the vaccine batches.</p>
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<li>France</li>
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<name sortKey="Lina, B" sort="Lina, B" uniqKey="Lina B" first="B." last="Lina">B. Lina</name>
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<name sortKey="Valette, M" sort="Valette, M" uniqKey="Valette M" first="M." last="Valette">M. Valette</name>
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   |wiki=    Sante
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   |texte=   Divergent genetic evolution of hemagglutinin in influenza A H1N1 and A H1N2 subtypes isolated in the south-France since the winter of 2001-2002.
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