Differential sensitivity of human, avian, and equine influenza a viruses to a glycoprotein inhibitor of infection: Selection of receptor specific variants
Identifieur interne : 002597 ( Main/Exploration ); précédent : 002596; suivant : 002598Differential sensitivity of human, avian, and equine influenza a viruses to a glycoprotein inhibitor of infection: Selection of receptor specific variants
Auteurs : Gary N. Rogers [États-Unis] ; Thomas J. Pritchett [États-Unis] ; Jeri L. Lane [États-Unis] ; James C. Paulson [États-Unis]Source :
- Virology [ 0042-6822 ] ; 1983.
English descriptors
- Teeft :
- Academic press, Adsorption, Adsorption period, Agglutinated, Agglutinated erythrocytes, Amino acid, Asialo, Assay, Avian, Binding properties, Cell lysates, Cell surface, Cell surface receptors, Choppin, Clone, Derivatized, Derivatized erythrocytes, Determinant, Enzymatically, Equine, Erythrocyte, Glycoprotein, Glycoprotein inhibitor, Hemagglutinating units, Hemagglutination, Hemagglutination inhibition, Hemagglutinin, Hemagglutinins, Hong kong, Horse serum, Human virus, Influenza, Influenza virus, Influenza viruses, Inhibitor, Inhibitor sensitivity, Laboratory passage, Laver, Linkage, Mdck, Mdck cells, Native erythrocytes, Neuraminidase, Normal horse serum, Oligosaccharide, Paulson, Phenotype, Plaque, Preferential binding, Receptor, Receptor determinants, Receptor specificities, Receptor specificity, Receptor variants, Room temperature, Selective pressures, Serum, Sialic, Sialic acid, Sialyloligosaccharide structures, Sialyloligosaccharides, Specific viruses, Structural relationships, Subtypes, Tamm, Unpublished results, Variant, Viral, Viral adsorption, Viral hemagglutinins, Viral neuraminidase, Virus, Virus particles, Virus population, Virus strains, Virus subtypes, World health organization.
Abstract
Abstract: Human and animal (avian and equine) influenza A virus isolates of the H3 serotype exhibit marked differences in their ability to bind specific sialyloligosaccharide sequences that serve as cell surface receptor determinants. (G. Rogers and J. Paulson, 1983, Virology 127, 361–373). Whereas human isolates of this subtype strongly agglutinate enzymatically modified human erythrocytes containign the terminal SAα2,6Gal sequence, avian and equine isolates preferentially agglutinate erythrocytes bearing the SAα2,3Gal sequence. As shown in this report, a glycoprotein found in horse serum, α2-macroglobulin, is a potent inhibitor of viral adsorption to the cell surface for human H3 isolates. In contrast, avian and equine isolates are poorly inhibited suggesting a correlation between receptor specificity and inhibitor sensitivity. Growth of a human H3 isolate (A/Memphis/102/72) on MDCK cells in the presence of horse serum resulted in an overall shift in the virus receptor specificity from preferential binding of the SAα2,6Gal linkage to preferential binding of the SAα2,3Gal linkage characteristic of avian and equine isolates. Clonally isolated variants of A/Memphis/102/72 grown in the presence or absence of horse serum exhibited binding properties that account for those observed in the file disolates. Clones which preferentially bound the SAα2,6Gal linkage, like the parent human virus, were very sensitive to inhibition of hemagglutination by horse serum and equine α2-macroglobulin. In contrast, receptor variants which preferentially bound the SAα2,3Gal linkage, like the avian and equine isolate, were insensitive to such inhibitors. None of the variants was very sensitivie to inhibition of hemagglutination by human α2-macroglobulin. These results suggest that the presence, in vivo, of a glycoprotein inhibitor such as equine α2-macroglobulin could suppress infection of influenza viruses bearing an H3 hemagglutinin with a SAα2,6Gal specific, inhibitor sensitive phenotype, allowing gorwth to predominance of a virus which is SAα2,3Gal specific and inhibitor insensitive as found in avian and equine isolates.
Url:
DOI: 10.1016/0042-6822(83)90507-X
Affiliations:
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Paulson</name><affiliation wicri:level="1"><country xml:lang="fr">États-Unis</country><wicri:regionArea>Department of Biological Chemisry, UCLA School of Medicine, Los Angeles, California 90024</wicri:regionArea><wicri:noRegion>California 90024</wicri:noRegion></affiliation></author></analytic><monogr></monogr><series><title level="j">Virology</title><title level="j" type="abbrev">YVIRO</title><idno type="ISSN">0042-6822</idno><imprint><publisher>ELSEVIER</publisher><date type="published" when="1983">1983</date><biblScope unit="volume">131</biblScope><biblScope unit="issue">2</biblScope><biblScope unit="page" from="394">394</biblScope><biblScope unit="page" to="408">408</biblScope></imprint><idno type="ISSN">0042-6822</idno></series></biblStruct></sourceDesc><seriesStmt><idno type="ISSN">0042-6822</idno></seriesStmt></fileDesc><profileDesc><textClass><keywords scheme="Teeft" xml:lang="en"><term>Academic press</term><term>Adsorption</term><term>Adsorption period</term><term>Agglutinated</term><term>Agglutinated erythrocytes</term><term>Amino acid</term><term>Asialo</term><term>Assay</term><term>Avian</term><term>Binding properties</term><term>Cell lysates</term><term>Cell surface</term><term>Cell surface receptors</term><term>Choppin</term><term>Clone</term><term>Derivatized</term><term>Derivatized erythrocytes</term><term>Determinant</term><term>Enzymatically</term><term>Equine</term><term>Erythrocyte</term><term>Glycoprotein</term><term>Glycoprotein inhibitor</term><term>Hemagglutinating units</term><term>Hemagglutination</term><term>Hemagglutination inhibition</term><term>Hemagglutinin</term><term>Hemagglutinins</term><term>Hong kong</term><term>Horse serum</term><term>Human virus</term><term>Influenza</term><term>Influenza virus</term><term>Influenza viruses</term><term>Inhibitor</term><term>Inhibitor sensitivity</term><term>Laboratory passage</term><term>Laver</term><term>Linkage</term><term>Mdck</term><term>Mdck cells</term><term>Native erythrocytes</term><term>Neuraminidase</term><term>Normal horse serum</term><term>Oligosaccharide</term><term>Paulson</term><term>Phenotype</term><term>Plaque</term><term>Preferential binding</term><term>Receptor</term><term>Receptor determinants</term><term>Receptor specificities</term><term>Receptor specificity</term><term>Receptor variants</term><term>Room temperature</term><term>Selective pressures</term><term>Serum</term><term>Sialic</term><term>Sialic acid</term><term>Sialyloligosaccharide structures</term><term>Sialyloligosaccharides</term><term>Specific viruses</term><term>Structural relationships</term><term>Subtypes</term><term>Tamm</term><term>Unpublished results</term><term>Variant</term><term>Viral</term><term>Viral adsorption</term><term>Viral hemagglutinins</term><term>Viral neuraminidase</term><term>Virus</term><term>Virus particles</term><term>Virus population</term><term>Virus strains</term><term>Virus subtypes</term><term>World health organization</term></keywords></textClass><langUsage><language ident="en">en</language></langUsage></profileDesc></teiHeader><front><div type="abstract" xml:lang="en">Abstract: Human and animal (avian and equine) influenza A virus isolates of the H3 serotype exhibit marked differences in their ability to bind specific sialyloligosaccharide sequences that serve as cell surface receptor determinants. (G. Rogers and J. Paulson, 1983, Virology 127, 361–373). Whereas human isolates of this subtype strongly agglutinate enzymatically modified human erythrocytes containign the terminal SAα2,6Gal sequence, avian and equine isolates preferentially agglutinate erythrocytes bearing the SAα2,3Gal sequence. As shown in this report, a glycoprotein found in horse serum, α2-macroglobulin, is a potent inhibitor of viral adsorption to the cell surface for human H3 isolates. In contrast, avian and equine isolates are poorly inhibited suggesting a correlation between receptor specificity and inhibitor sensitivity. Growth of a human H3 isolate (A/Memphis/102/72) on MDCK cells in the presence of horse serum resulted in an overall shift in the virus receptor specificity from preferential binding of the SAα2,6Gal linkage to preferential binding of the SAα2,3Gal linkage characteristic of avian and equine isolates. Clonally isolated variants of A/Memphis/102/72 grown in the presence or absence of horse serum exhibited binding properties that account for those observed in the file disolates. Clones which preferentially bound the SAα2,6Gal linkage, like the parent human virus, were very sensitive to inhibition of hemagglutination by horse serum and equine α2-macroglobulin. In contrast, receptor variants which preferentially bound the SAα2,3Gal linkage, like the avian and equine isolate, were insensitive to such inhibitors. None of the variants was very sensitivie to inhibition of hemagglutination by human α2-macroglobulin. These results suggest that the presence, in vivo, of a glycoprotein inhibitor such as equine α2-macroglobulin could suppress infection of influenza viruses bearing an H3 hemagglutinin with a SAα2,6Gal specific, inhibitor sensitive phenotype, allowing gorwth to predominance of a virus which is SAα2,3Gal specific and inhibitor insensitive as found in avian and equine isolates.</div></front></TEI><affiliations><list><country><li>États-Unis</li></country></list><tree><country name="États-Unis"><noRegion><name sortKey="Rogers, Gary N" sort="Rogers, Gary N" uniqKey="Rogers G" first="Gary N." last="Rogers">Gary N. Rogers</name></noRegion><name sortKey="Lane, Jeri L" sort="Lane, Jeri L" uniqKey="Lane J" first="Jeri L." last="Lane">Jeri L. Lane</name><name sortKey="Paulson, James C" sort="Paulson, James C" uniqKey="Paulson J" first="James C." last="Paulson">James C. Paulson</name><name sortKey="Pritchett, Thomas J" sort="Pritchett, Thomas J" uniqKey="Pritchett T" first="Thomas J." last="Pritchett">Thomas J. Pritchett</name></country></tree></affiliations></record>Pour manipuler ce document sous Unix (Dilib)
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