Study of Vaccinia and Cowpox viruses' replication in Rac1-N17 dominant-negative cells
Interfering with cellular signal transduction pathways is a common strategy used by many viruses to create a propitious intracellular environment for an efficient replication. Our group has been studying cellular signalling pathways activated by the orthopoxviruses Vaccinia (VACV) and Cowpox (CPXV)...
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Instituto Oswaldo Cruz, Ministério da Saúde
2013-08-01
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doaj-113c91f1bbce4fbda0c53e61e2a0cf372020-11-25T00:13:20ZengInstituto Oswaldo Cruz, Ministério da SaúdeMemórias do Instituto Oswaldo Cruz.1678-80602013-08-01108555456210.1590/S0074-02762013000500004S0074-02762013000500554Study of Vaccinia and Cowpox viruses' replication in Rac1-N17 dominant-negative cellsAna Paula Carneiro SalgadoJamária Adriana Pinheiro Soares-MartinsLuciana Garcia AndradeJonas Dutra AlbarnazPaulo César Peregrino FerreiraErna Geessien KroonCláudio Antônio BonjardimInterfering with cellular signal transduction pathways is a common strategy used by many viruses to create a propitious intracellular environment for an efficient replication. Our group has been studying cellular signalling pathways activated by the orthopoxviruses Vaccinia (VACV) and Cowpox (CPXV) and their significance to viral replication. In the present study our aim was to investigate whether the GTPase Rac1 was an upstream signal that led to the activation of MEK/ERK1/2, JNK1/2 or Akt pathways upon VACV or CPXV' infections. Therefore, we generated stable murine fibroblasts exhibiting negative dominance to Rac1-N17 to evaluate viral growth and the phosphorylation status of ERK1/2, JNK1/2 and Akt. Our results demonstrated that VACV replication, but not CPXV, was affected in dominant-negative (DN) Rac1-N17 cell lines in which viral yield was reduced in about 10-fold. Viral late gene expression, but not early, was also reduced. Furthermore, our data showed that Akt phosphorylation was diminished upon VACV infection in DN Rac1-N17 cells, suggesting that Rac1 participates in the phosphoinositide-3 kinase pathway leading to the activation of Akt. In conclusion, our results indicate that while Rac1 indeed plays a role in VACV biology, perhaps another GTPase may be involved in CPXV replication.http://www.scielo.br/scielo.php?script=sci_arttext&pid=S0074-02762013000500554&lng=en&tlng=enRac1AktVaccinia virusCowpox virusvirus-host interaction |
collection |
DOAJ |
language |
English |
format |
Article |
sources |
DOAJ |
author |
Ana Paula Carneiro Salgado Jamária Adriana Pinheiro Soares-Martins Luciana Garcia Andrade Jonas Dutra Albarnaz Paulo César Peregrino Ferreira Erna Geessien Kroon Cláudio Antônio Bonjardim |
spellingShingle |
Ana Paula Carneiro Salgado Jamária Adriana Pinheiro Soares-Martins Luciana Garcia Andrade Jonas Dutra Albarnaz Paulo César Peregrino Ferreira Erna Geessien Kroon Cláudio Antônio Bonjardim Study of Vaccinia and Cowpox viruses' replication in Rac1-N17 dominant-negative cells Memórias do Instituto Oswaldo Cruz. Rac1 Akt Vaccinia virus Cowpox virus virus-host interaction |
author_facet |
Ana Paula Carneiro Salgado Jamária Adriana Pinheiro Soares-Martins Luciana Garcia Andrade Jonas Dutra Albarnaz Paulo César Peregrino Ferreira Erna Geessien Kroon Cláudio Antônio Bonjardim |
author_sort |
Ana Paula Carneiro Salgado |
title |
Study of Vaccinia and Cowpox viruses' replication in Rac1-N17 dominant-negative cells |
title_short |
Study of Vaccinia and Cowpox viruses' replication in Rac1-N17 dominant-negative cells |
title_full |
Study of Vaccinia and Cowpox viruses' replication in Rac1-N17 dominant-negative cells |
title_fullStr |
Study of Vaccinia and Cowpox viruses' replication in Rac1-N17 dominant-negative cells |
title_full_unstemmed |
Study of Vaccinia and Cowpox viruses' replication in Rac1-N17 dominant-negative cells |
title_sort |
study of vaccinia and cowpox viruses' replication in rac1-n17 dominant-negative cells |
publisher |
Instituto Oswaldo Cruz, Ministério da Saúde |
series |
Memórias do Instituto Oswaldo Cruz. |
issn |
1678-8060 |
publishDate |
2013-08-01 |
description |
Interfering with cellular signal transduction pathways is a common strategy used by many viruses to create a propitious intracellular environment for an efficient replication. Our group has been studying cellular signalling pathways activated by the orthopoxviruses Vaccinia (VACV) and Cowpox (CPXV) and their significance to viral replication. In the present study our aim was to investigate whether the GTPase Rac1 was an upstream signal that led to the activation of MEK/ERK1/2, JNK1/2 or Akt pathways upon VACV or CPXV' infections. Therefore, we generated stable murine fibroblasts exhibiting negative dominance to Rac1-N17 to evaluate viral growth and the phosphorylation status of ERK1/2, JNK1/2 and Akt. Our results demonstrated that VACV replication, but not CPXV, was affected in dominant-negative (DN) Rac1-N17 cell lines in which viral yield was reduced in about 10-fold. Viral late gene expression, but not early, was also reduced. Furthermore, our data showed that Akt phosphorylation was diminished upon VACV infection in DN Rac1-N17 cells, suggesting that Rac1 participates in the phosphoinositide-3 kinase pathway leading to the activation of Akt. In conclusion, our results indicate that while Rac1 indeed plays a role in VACV biology, perhaps another GTPase may be involved in CPXV replication. |
topic |
Rac1 Akt Vaccinia virus Cowpox virus virus-host interaction |
url |
http://www.scielo.br/scielo.php?script=sci_arttext&pid=S0074-02762013000500554&lng=en&tlng=en |
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