Amino acid substitutions in the non-structural proteins 4A or 4B modulate the induction of autophagy in West Nile virus infected cells independently of the activation of the unfolded protein response

Amino acid substitutions in the non-structural proteins 4A or 4B modulate the induction of autophagy in West Nile virus infected cells independently of the activation of the unfolded protein response

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West Nile virus (WNV) is a neurotropic mosquito-borne flavivirus responsible for outbreaks of meningitis and encephalitis. Whereas the activation of autophagy in cells infected with other flaviviruses is well known, the interaction of WNV with the autophagic pathway still remains unclear and there are reports describing opposite findings obtained even analyzing the same viral strain. To clarify this controversy, we first analyzed the induction of autophagic features in cells infected with a panel of WNV strains. WNV was determined to induce autophagy in a strain dependent manner. We observed that all WNV strains or isolates analyzed, except for the WNV NY99 used, upregulated the autophagic pathway in infected cells. Interestingly, a variant derived from this WNV NY99 isolated from a persistently infected mouse increased LC3 modification and aggregation. Genome sequencing of this variant revealed only two non-synonymous nucleotide substitutions when compared to parental NY99 strain. These nucleotide substitutions introduced one amino acid replacement in NS4A and other in NS4B. Using genetically engineered viruses we showed that introduction of only one of these replacements was sufficient to upregulate the autophagic pathway. Thus, in this work we have shown that naturally occurring point mutations in the viral non structural proteins NS4A and NS4B confer WNV with the ability to induce the hallmarks of autophagy such as LC3 modification and aggregation. Even more, the differences on the induction of an autophagic response observed among WNV variants in infected cells did not correlate with alterations on the activation of the unfolded protein response (UPR), suggesting an uncoupling of UPR and autophagy during flavivirus infection. The findings here reported could help to improve the knowledge of the cellular processes involved on flavivirus-host cell interactions and contribute to the design of effective strategies to combat these pathogens.

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Bibliographic Details
Main Authors: Blázquez Martín, Ana Belén, Martín-Acebes, M. A., Saiz Calahorra, Juan Carlos
Format: artículo biblioteca
Language:English
Published: Frontiers Media 2014
Subjects:Autophagy, LC3, West Nile virus (WNV), Replication, Host cells, Unfolded protein response,
Online Access:http://hdl.handle.net/20.500.12792/3963
http://hdl.handle.net/10261/290144
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spelling dig-inia-es-10261-2901442023-02-17T08:27:51Z Amino acid substitutions in the non-structural proteins 4A or 4B modulate the induction of autophagy in West Nile virus infected cells independently of the activation of the unfolded protein response Blázquez Martín, Ana Belén Martín-Acebes, M. A. Saiz Calahorra, Juan Carlos Autophagy LC3 West Nile virus (WNV) Replication Host cells Unfolded protein response West Nile virus (WNV) is a neurotropic mosquito-borne flavivirus responsible for outbreaks of meningitis and encephalitis. Whereas the activation of autophagy in cells infected with other flaviviruses is well known, the interaction of WNV with the autophagic pathway still remains unclear and there are reports describing opposite findings obtained even analyzing the same viral strain. To clarify this controversy, we first analyzed the induction of autophagic features in cells infected with a panel of WNV strains. WNV was determined to induce autophagy in a strain dependent manner. We observed that all WNV strains or isolates analyzed, except for the WNV NY99 used, upregulated the autophagic pathway in infected cells. Interestingly, a variant derived from this WNV NY99 isolated from a persistently infected mouse increased LC3 modification and aggregation. Genome sequencing of this variant revealed only two non-synonymous nucleotide substitutions when compared to parental NY99 strain. These nucleotide substitutions introduced one amino acid replacement in NS4A and other in NS4B. Using genetically engineered viruses we showed that introduction of only one of these replacements was sufficient to upregulate the autophagic pathway. Thus, in this work we have shown that naturally occurring point mutations in the viral non structural proteins NS4A and NS4B confer WNV with the ability to induce the hallmarks of autophagy such as LC3 modification and aggregation. Even more, the differences on the induction of an autophagic response observed among WNV variants in infected cells did not correlate with alterations on the activation of the unfolded protein response (UPR), suggesting an uncoupling of UPR and autophagy during flavivirus infection. The findings here reported could help to improve the knowledge of the cellular processes involved on flavivirus-host cell interactions and contribute to the design of effective strategies to combat these pathogens. 2023-02-17T08:27:51Z 2023-02-17T08:27:51Z 2014 artículo Frontiers in Microbiology 5: e797 (2014) http://hdl.handle.net/20.500.12792/3963 http://hdl.handle.net/10261/290144 10.3389/fmicb.2014.00797 1664-302X en open Frontiers Media
institution INIA ES
collection DSpace
country España
countrycode ES
component Bibliográfico
access En linea
databasecode dig-inia-es
tag biblioteca
region Europa del Sur
libraryname Biblioteca del INIA España
language English
topic Autophagy
LC3
West Nile virus (WNV)
Replication
Host cells
Unfolded protein response
Autophagy
LC3
West Nile virus (WNV)
Replication
Host cells
Unfolded protein response
spellingShingle Autophagy
LC3
West Nile virus (WNV)
Replication
Host cells
Unfolded protein response
Autophagy
LC3
West Nile virus (WNV)
Replication
Host cells
Unfolded protein response
Blázquez Martín, Ana Belén
Martín-Acebes, M. A.
Saiz Calahorra, Juan Carlos
Amino acid substitutions in the non-structural proteins 4A or 4B modulate the induction of autophagy in West Nile virus infected cells independently of the activation of the unfolded protein response
description West Nile virus (WNV) is a neurotropic mosquito-borne flavivirus responsible for outbreaks of meningitis and encephalitis. Whereas the activation of autophagy in cells infected with other flaviviruses is well known, the interaction of WNV with the autophagic pathway still remains unclear and there are reports describing opposite findings obtained even analyzing the same viral strain. To clarify this controversy, we first analyzed the induction of autophagic features in cells infected with a panel of WNV strains. WNV was determined to induce autophagy in a strain dependent manner. We observed that all WNV strains or isolates analyzed, except for the WNV NY99 used, upregulated the autophagic pathway in infected cells. Interestingly, a variant derived from this WNV NY99 isolated from a persistently infected mouse increased LC3 modification and aggregation. Genome sequencing of this variant revealed only two non-synonymous nucleotide substitutions when compared to parental NY99 strain. These nucleotide substitutions introduced one amino acid replacement in NS4A and other in NS4B. Using genetically engineered viruses we showed that introduction of only one of these replacements was sufficient to upregulate the autophagic pathway. Thus, in this work we have shown that naturally occurring point mutations in the viral non structural proteins NS4A and NS4B confer WNV with the ability to induce the hallmarks of autophagy such as LC3 modification and aggregation. Even more, the differences on the induction of an autophagic response observed among WNV variants in infected cells did not correlate with alterations on the activation of the unfolded protein response (UPR), suggesting an uncoupling of UPR and autophagy during flavivirus infection. The findings here reported could help to improve the knowledge of the cellular processes involved on flavivirus-host cell interactions and contribute to the design of effective strategies to combat these pathogens.
format artículo
topic_facet Autophagy
LC3
West Nile virus (WNV)
Replication
Host cells
Unfolded protein response
author Blázquez Martín, Ana Belén
Martín-Acebes, M. A.
Saiz Calahorra, Juan Carlos
author_facet Blázquez Martín, Ana Belén
Martín-Acebes, M. A.
Saiz Calahorra, Juan Carlos
author_sort Blázquez Martín, Ana Belén
title Amino acid substitutions in the non-structural proteins 4A or 4B modulate the induction of autophagy in West Nile virus infected cells independently of the activation of the unfolded protein response
title_short Amino acid substitutions in the non-structural proteins 4A or 4B modulate the induction of autophagy in West Nile virus infected cells independently of the activation of the unfolded protein response
title_full Amino acid substitutions in the non-structural proteins 4A or 4B modulate the induction of autophagy in West Nile virus infected cells independently of the activation of the unfolded protein response
title_fullStr Amino acid substitutions in the non-structural proteins 4A or 4B modulate the induction of autophagy in West Nile virus infected cells independently of the activation of the unfolded protein response
title_full_unstemmed Amino acid substitutions in the non-structural proteins 4A or 4B modulate the induction of autophagy in West Nile virus infected cells independently of the activation of the unfolded protein response
title_sort amino acid substitutions in the non-structural proteins 4a or 4b modulate the induction of autophagy in west nile virus infected cells independently of the activation of the unfolded protein response
publisher Frontiers Media
publishDate 2014
url http://hdl.handle.net/20.500.12792/3963
http://hdl.handle.net/10261/290144
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AT martinacebesma aminoacidsubstitutionsinthenonstructuralproteins4aor4bmodulatetheinductionofautophagyinwestnilevirusinfectedcellsindependentlyoftheactivationoftheunfoldedproteinresponse
AT saizcalahorrajuancarlos aminoacidsubstitutionsinthenonstructuralproteins4aor4bmodulatetheinductionofautophagyinwestnilevirusinfectedcellsindependentlyoftheactivationoftheunfoldedproteinresponse
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