Effect of fusion protein cleavage site sequence on generation of a genotype VII Newcastle disease virus vaccine.

Newcastle disease (ND) causes severe economic loss to poultry industry worldwide. Frequent outbreaks of ND in commercial chickens vaccinated with live vaccines suggest a need to develop improved vaccines that are genetically matched against circulating Newcastle disease virus (NDV) strains. In this...

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Main Authors: Vinoth K Manoharan, Berin P Varghese, Anandan Paldurai, Siba K Samal
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2018-01-01
Series:PLoS ONE
Online Access:http://europepmc.org/articles/PMC5951571?pdf=render
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spelling doaj-f1701a4d0d2a4f77851ea406319c61462020-11-25T02:23:08ZengPublic Library of Science (PLoS)PLoS ONE1932-62032018-01-01135e019725310.1371/journal.pone.0197253Effect of fusion protein cleavage site sequence on generation of a genotype VII Newcastle disease virus vaccine.Vinoth K ManoharanBerin P VargheseAnandan PalduraiSiba K SamalNewcastle disease (ND) causes severe economic loss to poultry industry worldwide. Frequent outbreaks of ND in commercial chickens vaccinated with live vaccines suggest a need to develop improved vaccines that are genetically matched against circulating Newcastle disease virus (NDV) strains. In this study, the fusion protein cleavage site (FPCS) sequence of NDV strain Banjarmasin/010 (Banj), a genotype VII NDV, was individually modified using primer mutagenesis to those of avian paramyxovirus (APMV) serotypes 2, 7 and 8 and compared with the recombinant Banjarmasin (rBanj) with avirulent NDV LaSota cleavage site (rBanj-LaSota). These FPCS mutations changed the in vitro cell-to-cell fusion activity and made rBanj FPCS mutant viruses highly attenuated in chickens. When chickens immunized with the rBanj FPCS mutant viruses and challenged with the virulent Banj, there was reduced challenge virus shedding observed compared to chickens immunized with the heterologous vaccine strain LaSota. Among the genotype VII NDV Banj vaccine candidates, rBanj-LaSota and rBanj containing FPCS of APMV-8 induced highest neutralizing antibody titers and protected chickens with reduced challenge virus shedding. These results show the effect of the F protein cleavage site sequence in generating genotype VII matched NDV vaccines.http://europepmc.org/articles/PMC5951571?pdf=render
collection DOAJ
language English
format Article
sources DOAJ
author Vinoth K Manoharan
Berin P Varghese
Anandan Paldurai
Siba K Samal
spellingShingle Vinoth K Manoharan
Berin P Varghese
Anandan Paldurai
Siba K Samal
Effect of fusion protein cleavage site sequence on generation of a genotype VII Newcastle disease virus vaccine.
PLoS ONE
author_facet Vinoth K Manoharan
Berin P Varghese
Anandan Paldurai
Siba K Samal
author_sort Vinoth K Manoharan
title Effect of fusion protein cleavage site sequence on generation of a genotype VII Newcastle disease virus vaccine.
title_short Effect of fusion protein cleavage site sequence on generation of a genotype VII Newcastle disease virus vaccine.
title_full Effect of fusion protein cleavage site sequence on generation of a genotype VII Newcastle disease virus vaccine.
title_fullStr Effect of fusion protein cleavage site sequence on generation of a genotype VII Newcastle disease virus vaccine.
title_full_unstemmed Effect of fusion protein cleavage site sequence on generation of a genotype VII Newcastle disease virus vaccine.
title_sort effect of fusion protein cleavage site sequence on generation of a genotype vii newcastle disease virus vaccine.
publisher Public Library of Science (PLoS)
series PLoS ONE
issn 1932-6203
publishDate 2018-01-01
description Newcastle disease (ND) causes severe economic loss to poultry industry worldwide. Frequent outbreaks of ND in commercial chickens vaccinated with live vaccines suggest a need to develop improved vaccines that are genetically matched against circulating Newcastle disease virus (NDV) strains. In this study, the fusion protein cleavage site (FPCS) sequence of NDV strain Banjarmasin/010 (Banj), a genotype VII NDV, was individually modified using primer mutagenesis to those of avian paramyxovirus (APMV) serotypes 2, 7 and 8 and compared with the recombinant Banjarmasin (rBanj) with avirulent NDV LaSota cleavage site (rBanj-LaSota). These FPCS mutations changed the in vitro cell-to-cell fusion activity and made rBanj FPCS mutant viruses highly attenuated in chickens. When chickens immunized with the rBanj FPCS mutant viruses and challenged with the virulent Banj, there was reduced challenge virus shedding observed compared to chickens immunized with the heterologous vaccine strain LaSota. Among the genotype VII NDV Banj vaccine candidates, rBanj-LaSota and rBanj containing FPCS of APMV-8 induced highest neutralizing antibody titers and protected chickens with reduced challenge virus shedding. These results show the effect of the F protein cleavage site sequence in generating genotype VII matched NDV vaccines.
url http://europepmc.org/articles/PMC5951571?pdf=render
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