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Identification of H3N2 NA and PB1-F2 genetic variants and their association with disease symptoms during the 2014–15 influenza season

The 2014–15 influenza season saw the emergence of an H3N2 antigenic drift variant that formed the 3C.2a HA clade. Whole viral genomes were sequenced from nasopharyngeal swabs of ninety-four patients with confirmed influenza A virus infection and primary human nasal epithelial cell cultures used to e...

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Autores principales: Blumenkrantz, Deena R, Mehoke, Thomas, Shaw-Saliba, Kathryn, Powell, Harrison, Wohlgemuth, Nicholas, Liu, Hsuan, Macias, Elizabeth, Evans, Jared, Lewis, Mitra, Medina, Rebecca, Hardick, Justin, Sauer, Lauren M, Dugas, Andrea, DuVal, Anna, Lane, Andrew P, Gaydos, Charlotte, Rothman, Richard, Thielen, Peter, Pekosz, Andrew
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Oxford University Press 2021
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8197029/
https://www.ncbi.nlm.nih.gov/pubmed/34131512
http://dx.doi.org/10.1093/ve/veab047
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author Blumenkrantz, Deena R
Mehoke, Thomas
Shaw-Saliba, Kathryn
Powell, Harrison
Wohlgemuth, Nicholas
Liu, Hsuan
Macias, Elizabeth
Evans, Jared
Lewis, Mitra
Medina, Rebecca
Hardick, Justin
Sauer, Lauren M
Dugas, Andrea
DuVal, Anna
Lane, Andrew P
Gaydos, Charlotte
Rothman, Richard
Thielen, Peter
Pekosz, Andrew
author_facet Blumenkrantz, Deena R
Mehoke, Thomas
Shaw-Saliba, Kathryn
Powell, Harrison
Wohlgemuth, Nicholas
Liu, Hsuan
Macias, Elizabeth
Evans, Jared
Lewis, Mitra
Medina, Rebecca
Hardick, Justin
Sauer, Lauren M
Dugas, Andrea
DuVal, Anna
Lane, Andrew P
Gaydos, Charlotte
Rothman, Richard
Thielen, Peter
Pekosz, Andrew
author_sort Blumenkrantz, Deena R
collection PubMed
description The 2014–15 influenza season saw the emergence of an H3N2 antigenic drift variant that formed the 3C.2a HA clade. Whole viral genomes were sequenced from nasopharyngeal swabs of ninety-four patients with confirmed influenza A virus infection and primary human nasal epithelial cell cultures used to efficiently isolate H3N2 viruses. The isolates were classified by HA clade and the presence of a new set of co-selected mutations in NA (a glycosylation site, NAg+) and PB1-F2 (H75P). The NA and PB1-F2 mutations were present in a subset of clade 3C.2a viruses (NAg+F2P), which dominated during the subsequent influenza seasons. In human nasal epithelial cell cultures, a virus with the novel NAg+F2P genotype replicated less well compared with a virus with the parental genotype. Retrospective analyses of clinical data showed that NAg+F2P genotype viruses were associated with increased cough and shortness of breath in infected patients.
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spelling pubmed-81970292021-06-14 Identification of H3N2 NA and PB1-F2 genetic variants and their association with disease symptoms during the 2014–15 influenza season Blumenkrantz, Deena R Mehoke, Thomas Shaw-Saliba, Kathryn Powell, Harrison Wohlgemuth, Nicholas Liu, Hsuan Macias, Elizabeth Evans, Jared Lewis, Mitra Medina, Rebecca Hardick, Justin Sauer, Lauren M Dugas, Andrea DuVal, Anna Lane, Andrew P Gaydos, Charlotte Rothman, Richard Thielen, Peter Pekosz, Andrew Virus Evol Research Article The 2014–15 influenza season saw the emergence of an H3N2 antigenic drift variant that formed the 3C.2a HA clade. Whole viral genomes were sequenced from nasopharyngeal swabs of ninety-four patients with confirmed influenza A virus infection and primary human nasal epithelial cell cultures used to efficiently isolate H3N2 viruses. The isolates were classified by HA clade and the presence of a new set of co-selected mutations in NA (a glycosylation site, NAg+) and PB1-F2 (H75P). The NA and PB1-F2 mutations were present in a subset of clade 3C.2a viruses (NAg+F2P), which dominated during the subsequent influenza seasons. In human nasal epithelial cell cultures, a virus with the novel NAg+F2P genotype replicated less well compared with a virus with the parental genotype. Retrospective analyses of clinical data showed that NAg+F2P genotype viruses were associated with increased cough and shortness of breath in infected patients. Oxford University Press 2021-06-04 /pmc/articles/PMC8197029/ /pubmed/34131512 http://dx.doi.org/10.1093/ve/veab047 Text en © The Author(s) 2021. Published by Oxford University Press. https://creativecommons.org/licenses/by-nc/4.0/This is an Open Access article distributed under the terms of the Creative Commons Attribution Non-Commercial License (http://creativecommons.org/licenses/by-nc/4.0/ (https://creativecommons.org/licenses/by-nc/4.0/) ), which permits non-commercial re-use, distribution, and reproduction in any medium, provided the original work is properly cited. For commercial re-use, please contact journals.permissions@oup.com
spellingShingle Research Article
Blumenkrantz, Deena R
Mehoke, Thomas
Shaw-Saliba, Kathryn
Powell, Harrison
Wohlgemuth, Nicholas
Liu, Hsuan
Macias, Elizabeth
Evans, Jared
Lewis, Mitra
Medina, Rebecca
Hardick, Justin
Sauer, Lauren M
Dugas, Andrea
DuVal, Anna
Lane, Andrew P
Gaydos, Charlotte
Rothman, Richard
Thielen, Peter
Pekosz, Andrew
Identification of H3N2 NA and PB1-F2 genetic variants and their association with disease symptoms during the 2014–15 influenza season
title Identification of H3N2 NA and PB1-F2 genetic variants and their association with disease symptoms during the 2014–15 influenza season
title_full Identification of H3N2 NA and PB1-F2 genetic variants and their association with disease symptoms during the 2014–15 influenza season
title_fullStr Identification of H3N2 NA and PB1-F2 genetic variants and their association with disease symptoms during the 2014–15 influenza season
title_full_unstemmed Identification of H3N2 NA and PB1-F2 genetic variants and their association with disease symptoms during the 2014–15 influenza season
title_short Identification of H3N2 NA and PB1-F2 genetic variants and their association with disease symptoms during the 2014–15 influenza season
title_sort identification of h3n2 na and pb1-f2 genetic variants and their association with disease symptoms during the 2014–15 influenza season
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8197029/
https://www.ncbi.nlm.nih.gov/pubmed/34131512
http://dx.doi.org/10.1093/ve/veab047
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