MVA-based H5N1 vaccine affords cross-clade protection in mice against influenza A/H5N1 viruses at low doses and after single immunization.

MVA-based H5N1 vaccine affords cross-clade protection in mice against influenza A/H5N1 viruses at low doses and after single immunization.

Human infections with highly pathogenic avian influenza viruses of the H5N1 subtype, frequently reported since 2003, result in high morbidity and mortality. It is feared that these viruses become pandemic, therefore the development of safe and effective vaccines is desirable. MVA-based H5N1 vaccines...

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Autores principales: Joost H C M Kreijtz, Yasemin Suezer, Gerrie de Mutsert, Geert van Amerongen, Astrid Schwantes, Judith M A van den Brand, Ron A M Fouchier, Johannes Löwer, Albert D M E Osterhaus, Gerd Sutter, Guus F Rimmelzwaan
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Publicado: Public Library of Science (PLoS) 2009
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spelling oai:doaj.org-article:01ad0564450c46c4b13c74add8a2d0af2021-11-25T06:28:10ZMVA-based H5N1 vaccine affords cross-clade protection in mice against influenza A/H5N1 viruses at low doses and after single immunization.1932-620310.1371/journal.pone.0007790https://doaj.org/article/01ad0564450c46c4b13c74add8a2d0af2009-11-01T00:00:00Zhttps://www.ncbi.nlm.nih.gov/pmc/articles/pmid/19915662/pdf/?tool=EBIhttps://doaj.org/toc/1932-6203Human infections with highly pathogenic avian influenza viruses of the H5N1 subtype, frequently reported since 2003, result in high morbidity and mortality. It is feared that these viruses become pandemic, therefore the development of safe and effective vaccines is desirable. MVA-based H5N1 vaccines already proved to be effective when two immunizations with high doses were used. Dose-sparing strategies would increase the number of people that can be vaccinated when the amount of vaccine preparations that can be produced is limited. Furthermore, protective immunity is induced ideally after a single immunization. Therefore the minimal requirements for induction of protective immunity with a MVA-based H5N1 vaccine were assessed in mice. To this end, mice were vaccinated once or twice with descending doses of a recombinant MVA expressing the HA gene of influenza virus A/Vietnam/1194/04. The protective efficacy was determined after challenge infection with the homologous clade 1 virus and a heterologous virus derived from clade 2.1, A/Indonesia/5/05 by assessing weight loss, virus replication and histopathological changes. It was concluded that MVA-based vaccines allowed significant dose-sparing and afford cross-clade protection, also after a single immunization, which are favorable properties for an H5N1 vaccine candidate.Joost H C M KreijtzYasemin SuezerGerrie de MutsertGeert van AmerongenAstrid SchwantesJudith M A van den BrandRon A M FouchierJohannes LöwerAlbert D M E OsterhausGerd SutterGuus F RimmelzwaanPublic Library of Science (PLoS)articleMedicineRScienceQENPLoS ONE, Vol 4, Iss 11, p e7790 (2009)
institution DOAJ
collection DOAJ
language EN
topic Medicine
R
Science
Q
spellingShingle Medicine
R
Science
Q
Joost H C M Kreijtz
Yasemin Suezer
Gerrie de Mutsert
Geert van Amerongen
Astrid Schwantes
Judith M A van den Brand
Ron A M Fouchier
Johannes Löwer
Albert D M E Osterhaus
Gerd Sutter
Guus F Rimmelzwaan
MVA-based H5N1 vaccine affords cross-clade protection in mice against influenza A/H5N1 viruses at low doses and after single immunization.
description Human infections with highly pathogenic avian influenza viruses of the H5N1 subtype, frequently reported since 2003, result in high morbidity and mortality. It is feared that these viruses become pandemic, therefore the development of safe and effective vaccines is desirable. MVA-based H5N1 vaccines already proved to be effective when two immunizations with high doses were used. Dose-sparing strategies would increase the number of people that can be vaccinated when the amount of vaccine preparations that can be produced is limited. Furthermore, protective immunity is induced ideally after a single immunization. Therefore the minimal requirements for induction of protective immunity with a MVA-based H5N1 vaccine were assessed in mice. To this end, mice were vaccinated once or twice with descending doses of a recombinant MVA expressing the HA gene of influenza virus A/Vietnam/1194/04. The protective efficacy was determined after challenge infection with the homologous clade 1 virus and a heterologous virus derived from clade 2.1, A/Indonesia/5/05 by assessing weight loss, virus replication and histopathological changes. It was concluded that MVA-based vaccines allowed significant dose-sparing and afford cross-clade protection, also after a single immunization, which are favorable properties for an H5N1 vaccine candidate.
format article
author Joost H C M Kreijtz
Yasemin Suezer
Gerrie de Mutsert
Geert van Amerongen
Astrid Schwantes
Judith M A van den Brand
Ron A M Fouchier
Johannes Löwer
Albert D M E Osterhaus
Gerd Sutter
Guus F Rimmelzwaan
author_facet Joost H C M Kreijtz
Yasemin Suezer
Gerrie de Mutsert
Geert van Amerongen
Astrid Schwantes
Judith M A van den Brand
Ron A M Fouchier
Johannes Löwer
Albert D M E Osterhaus
Gerd Sutter
Guus F Rimmelzwaan
author_sort Joost H C M Kreijtz
title MVA-based H5N1 vaccine affords cross-clade protection in mice against influenza A/H5N1 viruses at low doses and after single immunization.
title_short MVA-based H5N1 vaccine affords cross-clade protection in mice against influenza A/H5N1 viruses at low doses and after single immunization.
title_full MVA-based H5N1 vaccine affords cross-clade protection in mice against influenza A/H5N1 viruses at low doses and after single immunization.
title_fullStr MVA-based H5N1 vaccine affords cross-clade protection in mice against influenza A/H5N1 viruses at low doses and after single immunization.
title_full_unstemmed MVA-based H5N1 vaccine affords cross-clade protection in mice against influenza A/H5N1 viruses at low doses and after single immunization.
title_sort mva-based h5n1 vaccine affords cross-clade protection in mice against influenza a/h5n1 viruses at low doses and after single immunization.
publisher Public Library of Science (PLoS)
publishDate 2009
url https://doaj.org/article/01ad0564450c46c4b13c74add8a2d0af
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