Mutations in the Schmallenberg Virus Gc Glycoprotein Facilitate Cellular Protein Synthesis Shutoff and Restore Pathogenicity of NSs Deletion Mutants in Mice

Serial passage of viruses in cell culture has been traditionally used to attenuate virulence and identify determinants of viral pathogenesis. In a previous study, we found that a strain of Schmallenberg virus (SBV) serially passaged in tissue culture (termed SBVp32) unexpectedly displayed increased...

Descripción completa

Detalles Bibliográficos
Autores principales: Varela, Mariana, Pinto, Rute Maria, Caporale, Marco, Piras, Ilaria M., Taggart, Aislynn, Seehusen, Frauke, Hahn, Kerstin, Janowicz, Anna, de Souza, William Marciel, Baumgärtner, Wolfgang, Shi, Xiaohong, Palmarini, Massimo
Formato: Online Artículo Texto
Lenguaje:English
Publicado: American Society for Microbiology 2016
Materias:
Pathogenesis and Immunity
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4934738/
https://www.ncbi.nlm.nih.gov/pubmed/26984728
http://dx.doi.org/10.1128/JVI.00424-16
_version_ 1782441383561265152
author Varela, Mariana
Pinto, Rute Maria
Caporale, Marco
Piras, Ilaria M.
Taggart, Aislynn
Seehusen, Frauke
Hahn, Kerstin
Janowicz, Anna
de Souza, William Marciel
Baumgärtner, Wolfgang
Shi, Xiaohong
Palmarini, Massimo
author_facet Varela, Mariana
Pinto, Rute Maria
Caporale, Marco
Piras, Ilaria M.
Taggart, Aislynn
Seehusen, Frauke
Hahn, Kerstin
Janowicz, Anna
de Souza, William Marciel
Baumgärtner, Wolfgang
Shi, Xiaohong
Palmarini, Massimo
author_sort Varela, Mariana
collection PubMed
description Serial passage of viruses in cell culture has been traditionally used to attenuate virulence and identify determinants of viral pathogenesis. In a previous study, we found that a strain of Schmallenberg virus (SBV) serially passaged in tissue culture (termed SBVp32) unexpectedly displayed increased pathogenicity in suckling mice compared to wild-type SBV. In this study, we mapped the determinants of SBVp32 virulence to the viral genome M segment. SBVp32 virulence is associated with the capacity of this virus to reach high titers in the brains of experimentally infected suckling mice. We also found that the Gc glycoprotein, encoded by the M segment of SBVp32, facilitates host cell protein shutoff in vitro. Interestingly, while the M segment of SBVp32 is a virulence factor, we found that the S segment of the same virus confers by itself an attenuated phenotype to wild-type SBV, as it has lost the ability to block the innate immune system of the host. Single mutations present in the Gc glycoprotein of SBVp32 are sufficient to compensate for both the attenuated phenotype of the SBVp32 S segment and the attenuated phenotype of NSs deletion mutants. Our data also indicate that the SBVp32 M segment does not act as an interferon (IFN) antagonist. Therefore, SBV mutants can retain pathogenicity even when they are unable to fully control the production of IFN by infected cells. Overall, this study suggests that the viral glycoprotein of orthobunyaviruses can compensate, at least in part, for the function of NSs. In addition, we also provide evidence that the induction of total cellular protein shutoff by SBV is determined by multiple viral proteins, while the ability to control the production of IFN maps to the NSs protein. IMPORTANCE The identification of viral determinants of pathogenesis is key to the development of prophylactic and intervention measures. In this study, we found that the bunyavirus Gc glycoprotein is a virulence factor. Importantly, we show that mutations in the Gc glycoprotein can restore the pathogenicity of attenuated mutants resulting from deletions or mutations in the nonstructural protein NSs. Our findings highlight the fact that careful consideration should be taken when designing live attenuated vaccines based on deletions of nonstructural proteins since single mutations in the viral glycoproteins appear to revert attenuated mutants to virulent phenotypes.
format Online
Article
Text
id pubmed-4934738
institution National Center for Biotechnology Information
language English
publishDate 2016
publisher American Society for Microbiology
record_format MEDLINE/PubMed
spelling pubmed-49347382016-07-26 Mutations in the Schmallenberg Virus Gc Glycoprotein Facilitate Cellular Protein Synthesis Shutoff and Restore Pathogenicity of NSs Deletion Mutants in Mice Varela, Mariana Pinto, Rute Maria Caporale, Marco Piras, Ilaria M. Taggart, Aislynn Seehusen, Frauke Hahn, Kerstin Janowicz, Anna de Souza, William Marciel Baumgärtner, Wolfgang Shi, Xiaohong Palmarini, Massimo J Virol Pathogenesis and Immunity Serial passage of viruses in cell culture has been traditionally used to attenuate virulence and identify determinants of viral pathogenesis. In a previous study, we found that a strain of Schmallenberg virus (SBV) serially passaged in tissue culture (termed SBVp32) unexpectedly displayed increased pathogenicity in suckling mice compared to wild-type SBV. In this study, we mapped the determinants of SBVp32 virulence to the viral genome M segment. SBVp32 virulence is associated with the capacity of this virus to reach high titers in the brains of experimentally infected suckling mice. We also found that the Gc glycoprotein, encoded by the M segment of SBVp32, facilitates host cell protein shutoff in vitro. Interestingly, while the M segment of SBVp32 is a virulence factor, we found that the S segment of the same virus confers by itself an attenuated phenotype to wild-type SBV, as it has lost the ability to block the innate immune system of the host. Single mutations present in the Gc glycoprotein of SBVp32 are sufficient to compensate for both the attenuated phenotype of the SBVp32 S segment and the attenuated phenotype of NSs deletion mutants. Our data also indicate that the SBVp32 M segment does not act as an interferon (IFN) antagonist. Therefore, SBV mutants can retain pathogenicity even when they are unable to fully control the production of IFN by infected cells. Overall, this study suggests that the viral glycoprotein of orthobunyaviruses can compensate, at least in part, for the function of NSs. In addition, we also provide evidence that the induction of total cellular protein shutoff by SBV is determined by multiple viral proteins, while the ability to control the production of IFN maps to the NSs protein. IMPORTANCE The identification of viral determinants of pathogenesis is key to the development of prophylactic and intervention measures. In this study, we found that the bunyavirus Gc glycoprotein is a virulence factor. Importantly, we show that mutations in the Gc glycoprotein can restore the pathogenicity of attenuated mutants resulting from deletions or mutations in the nonstructural protein NSs. Our findings highlight the fact that careful consideration should be taken when designing live attenuated vaccines based on deletions of nonstructural proteins since single mutations in the viral glycoproteins appear to revert attenuated mutants to virulent phenotypes. American Society for Microbiology 2016-05-12 /pmc/articles/PMC4934738/ /pubmed/26984728 http://dx.doi.org/10.1128/JVI.00424-16 Text en Copyright © 2016 Varela et al. http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution 4.0 International license (http://creativecommons.org/licenses/by/4.0/) .
spellingShingle Pathogenesis and Immunity
Varela, Mariana
Pinto, Rute Maria
Caporale, Marco
Piras, Ilaria M.
Taggart, Aislynn
Seehusen, Frauke
Hahn, Kerstin
Janowicz, Anna
de Souza, William Marciel
Baumgärtner, Wolfgang
Shi, Xiaohong
Palmarini, Massimo
Mutations in the Schmallenberg Virus Gc Glycoprotein Facilitate Cellular Protein Synthesis Shutoff and Restore Pathogenicity of NSs Deletion Mutants in Mice
title Mutations in the Schmallenberg Virus Gc Glycoprotein Facilitate Cellular Protein Synthesis Shutoff and Restore Pathogenicity of NSs Deletion Mutants in Mice
title_full Mutations in the Schmallenberg Virus Gc Glycoprotein Facilitate Cellular Protein Synthesis Shutoff and Restore Pathogenicity of NSs Deletion Mutants in Mice
title_fullStr Mutations in the Schmallenberg Virus Gc Glycoprotein Facilitate Cellular Protein Synthesis Shutoff and Restore Pathogenicity of NSs Deletion Mutants in Mice
title_full_unstemmed Mutations in the Schmallenberg Virus Gc Glycoprotein Facilitate Cellular Protein Synthesis Shutoff and Restore Pathogenicity of NSs Deletion Mutants in Mice
title_short Mutations in the Schmallenberg Virus Gc Glycoprotein Facilitate Cellular Protein Synthesis Shutoff and Restore Pathogenicity of NSs Deletion Mutants in Mice
title_sort mutations in the schmallenberg virus gc glycoprotein facilitate cellular protein synthesis shutoff and restore pathogenicity of nss deletion mutants in mice
topic Pathogenesis and Immunity
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4934738/
https://www.ncbi.nlm.nih.gov/pubmed/26984728
http://dx.doi.org/10.1128/JVI.00424-16
work_keys_str_mv AT varelamariana mutationsintheschmallenbergvirusgcglycoproteinfacilitatecellularproteinsynthesisshutoffandrestorepathogenicityofnssdeletionmutantsinmice
AT pintorutemaria mutationsintheschmallenbergvirusgcglycoproteinfacilitatecellularproteinsynthesisshutoffandrestorepathogenicityofnssdeletionmutantsinmice
AT caporalemarco mutationsintheschmallenbergvirusgcglycoproteinfacilitatecellularproteinsynthesisshutoffandrestorepathogenicityofnssdeletionmutantsinmice
AT pirasilariam mutationsintheschmallenbergvirusgcglycoproteinfacilitatecellularproteinsynthesisshutoffandrestorepathogenicityofnssdeletionmutantsinmice
AT taggartaislynn mutationsintheschmallenbergvirusgcglycoproteinfacilitatecellularproteinsynthesisshutoffandrestorepathogenicityofnssdeletionmutantsinmice
AT seehusenfrauke mutationsintheschmallenbergvirusgcglycoproteinfacilitatecellularproteinsynthesisshutoffandrestorepathogenicityofnssdeletionmutantsinmice
AT hahnkerstin mutationsintheschmallenbergvirusgcglycoproteinfacilitatecellularproteinsynthesisshutoffandrestorepathogenicityofnssdeletionmutantsinmice
AT janowiczanna mutationsintheschmallenbergvirusgcglycoproteinfacilitatecellularproteinsynthesisshutoffandrestorepathogenicityofnssdeletionmutantsinmice
AT desouzawilliammarciel mutationsintheschmallenbergvirusgcglycoproteinfacilitatecellularproteinsynthesisshutoffandrestorepathogenicityofnssdeletionmutantsinmice
AT baumgartnerwolfgang mutationsintheschmallenbergvirusgcglycoproteinfacilitatecellularproteinsynthesisshutoffandrestorepathogenicityofnssdeletionmutantsinmice
AT shixiaohong mutationsintheschmallenbergvirusgcglycoproteinfacilitatecellularproteinsynthesisshutoffandrestorepathogenicityofnssdeletionmutantsinmice
AT palmarinimassimo mutationsintheschmallenbergvirusgcglycoproteinfacilitatecellularproteinsynthesisshutoffandrestorepathogenicityofnssdeletionmutantsinmice

Ejemplares similares