The PKR activator, PACT, becomes a PKR inhibitor during HIV-1 replication

BACKGROUND: HIV-1 translation is modulated by the activation of the interferon (IFN)-inducible Protein Kinase RNA-activated (PKR). PKR phosphorylates its downstream targets, including the alpha subunit of the eukaryotic translation Initiation Factor 2 (eIF2α), which decreases viral replication. The...

Descripción completa

Detalles Bibliográficos
Autores principales: Clerzius, Guerline, Shaw, Eileen, Daher, Aïcha, Burugu, Samantha, Gélinas, Jean-François, Ear, Thornin, Sinck, Lucile, Routy, Jean-Pierre, Mouland, Andrew J, Patel, Rekha C, Gatignol, Anne
Formato: Online Artículo Texto
Lenguaje:English
Publicado: BioMed Central 2013
Materias:
Research
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3848765/
https://www.ncbi.nlm.nih.gov/pubmed/24020926
http://dx.doi.org/10.1186/1742-4690-10-96
_version_ 1782293816673304576
author Clerzius, Guerline
Shaw, Eileen
Daher, Aïcha
Burugu, Samantha
Gélinas, Jean-François
Ear, Thornin
Sinck, Lucile
Routy, Jean-Pierre
Mouland, Andrew J
Patel, Rekha C
Gatignol, Anne
author_facet Clerzius, Guerline
Shaw, Eileen
Daher, Aïcha
Burugu, Samantha
Gélinas, Jean-François
Ear, Thornin
Sinck, Lucile
Routy, Jean-Pierre
Mouland, Andrew J
Patel, Rekha C
Gatignol, Anne
author_sort Clerzius, Guerline
collection PubMed
description BACKGROUND: HIV-1 translation is modulated by the activation of the interferon (IFN)-inducible Protein Kinase RNA-activated (PKR). PKR phosphorylates its downstream targets, including the alpha subunit of the eukaryotic translation Initiation Factor 2 (eIF2α), which decreases viral replication. The PKR Activator (PACT) is known to activate PKR after a cellular stress. In lymphocytic cell lines, HIV-1 activates PKR only transiently and not when cells replicate the virus at high levels. The regulation of this activation is due to a combination of viral and cellular factors that have been only partially identified. RESULTS: PKR is transiently induced and activated in peripheral blood mononuclear cells after HIV-1 infection. The addition of IFN reduces viral replication, and induces both the production and phosphorylation of PKR. In lymphocytic Jurkat cells infected by HIV-1, a multiprotein complex around PKR contains the double-stranded RNA binding proteins (dsRBPs), adenosine deaminase acting on RNA (ADAR)1 and PACT. In HEK 293T cells transfected with an HIV-1 molecular clone, PACT unexpectedly inhibited PKR and eIF2α phosphorylation and increased HIV-1 protein expression and virion production in the presence of either endogenous PKR alone or overexpressed PKR. The comparison between different dsRBPs showed that ADAR1, TAR RNA Binding Protein (TRBP) and PACT inhibit PKR and eIF2α phosphorylation in HIV-infected cells, whereas Staufen1 did not. Individual or a combination of short hairpin RNAs against PACT or ADAR1 decreased HIV-1 protein expression. In the astrocytic cell line U251MG, which weakly expresses TRBP, PACT mediated an increased HIV-1 protein expression and a decreased PKR phosphorylation. In these cells, a truncated PACT, which constitutively activates PKR in non-infected cells showed no activity on either PKR or HIV-1 protein expression. Finally, PACT and ADAR1 interact with each other in the absence of RNAs. CONCLUSION: In contrast to its previously described activity, PACT contributes to PKR dephosphorylation during HIV-1 replication. This activity is in addition to its heterodimer formation with TRBP and could be due to its binding to ADAR1. HIV-1 has evolved to replicate in cells with high levels of TRBP, to induce the expression of ADAR1 and to change the function of PACT for PKR inhibition and increased replication.
format Online
Article
Text
id pubmed-3848765
institution National Center for Biotechnology Information
language English
publishDate 2013
publisher BioMed Central
record_format MEDLINE/PubMed
spelling pubmed-38487652013-12-04 The PKR activator, PACT, becomes a PKR inhibitor during HIV-1 replication Clerzius, Guerline Shaw, Eileen Daher, Aïcha Burugu, Samantha Gélinas, Jean-François Ear, Thornin Sinck, Lucile Routy, Jean-Pierre Mouland, Andrew J Patel, Rekha C Gatignol, Anne Retrovirology Research BACKGROUND: HIV-1 translation is modulated by the activation of the interferon (IFN)-inducible Protein Kinase RNA-activated (PKR). PKR phosphorylates its downstream targets, including the alpha subunit of the eukaryotic translation Initiation Factor 2 (eIF2α), which decreases viral replication. The PKR Activator (PACT) is known to activate PKR after a cellular stress. In lymphocytic cell lines, HIV-1 activates PKR only transiently and not when cells replicate the virus at high levels. The regulation of this activation is due to a combination of viral and cellular factors that have been only partially identified. RESULTS: PKR is transiently induced and activated in peripheral blood mononuclear cells after HIV-1 infection. The addition of IFN reduces viral replication, and induces both the production and phosphorylation of PKR. In lymphocytic Jurkat cells infected by HIV-1, a multiprotein complex around PKR contains the double-stranded RNA binding proteins (dsRBPs), adenosine deaminase acting on RNA (ADAR)1 and PACT. In HEK 293T cells transfected with an HIV-1 molecular clone, PACT unexpectedly inhibited PKR and eIF2α phosphorylation and increased HIV-1 protein expression and virion production in the presence of either endogenous PKR alone or overexpressed PKR. The comparison between different dsRBPs showed that ADAR1, TAR RNA Binding Protein (TRBP) and PACT inhibit PKR and eIF2α phosphorylation in HIV-infected cells, whereas Staufen1 did not. Individual or a combination of short hairpin RNAs against PACT or ADAR1 decreased HIV-1 protein expression. In the astrocytic cell line U251MG, which weakly expresses TRBP, PACT mediated an increased HIV-1 protein expression and a decreased PKR phosphorylation. In these cells, a truncated PACT, which constitutively activates PKR in non-infected cells showed no activity on either PKR or HIV-1 protein expression. Finally, PACT and ADAR1 interact with each other in the absence of RNAs. CONCLUSION: In contrast to its previously described activity, PACT contributes to PKR dephosphorylation during HIV-1 replication. This activity is in addition to its heterodimer formation with TRBP and could be due to its binding to ADAR1. HIV-1 has evolved to replicate in cells with high levels of TRBP, to induce the expression of ADAR1 and to change the function of PACT for PKR inhibition and increased replication. BioMed Central 2013-09-11 /pmc/articles/PMC3848765/ /pubmed/24020926 http://dx.doi.org/10.1186/1742-4690-10-96 Text en Copyright © 2013 Clerzius et al.; licensee BioMed Central Ltd. http://creativecommons.org/licenses/by/2.0 This is an Open Access article distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/2.0), which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.
spellingShingle Research
Clerzius, Guerline
Shaw, Eileen
Daher, Aïcha
Burugu, Samantha
Gélinas, Jean-François
Ear, Thornin
Sinck, Lucile
Routy, Jean-Pierre
Mouland, Andrew J
Patel, Rekha C
Gatignol, Anne
The PKR activator, PACT, becomes a PKR inhibitor during HIV-1 replication
title The PKR activator, PACT, becomes a PKR inhibitor during HIV-1 replication
title_full The PKR activator, PACT, becomes a PKR inhibitor during HIV-1 replication
title_fullStr The PKR activator, PACT, becomes a PKR inhibitor during HIV-1 replication
title_full_unstemmed The PKR activator, PACT, becomes a PKR inhibitor during HIV-1 replication
title_short The PKR activator, PACT, becomes a PKR inhibitor during HIV-1 replication
title_sort pkr activator, pact, becomes a pkr inhibitor during hiv-1 replication
topic Research
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3848765/
https://www.ncbi.nlm.nih.gov/pubmed/24020926
http://dx.doi.org/10.1186/1742-4690-10-96
work_keys_str_mv AT clerziusguerline thepkractivatorpactbecomesapkrinhibitorduringhiv1replication
AT shaweileen thepkractivatorpactbecomesapkrinhibitorduringhiv1replication
AT daheraicha thepkractivatorpactbecomesapkrinhibitorduringhiv1replication
AT burugusamantha thepkractivatorpactbecomesapkrinhibitorduringhiv1replication
AT gelinasjeanfrancois thepkractivatorpactbecomesapkrinhibitorduringhiv1replication
AT earthornin thepkractivatorpactbecomesapkrinhibitorduringhiv1replication
AT sincklucile thepkractivatorpactbecomesapkrinhibitorduringhiv1replication
AT routyjeanpierre thepkractivatorpactbecomesapkrinhibitorduringhiv1replication
AT moulandandrewj thepkractivatorpactbecomesapkrinhibitorduringhiv1replication
AT patelrekhac thepkractivatorpactbecomesapkrinhibitorduringhiv1replication
AT gatignolanne thepkractivatorpactbecomesapkrinhibitorduringhiv1replication
AT clerziusguerline pkractivatorpactbecomesapkrinhibitorduringhiv1replication
AT shaweileen pkractivatorpactbecomesapkrinhibitorduringhiv1replication
AT daheraicha pkractivatorpactbecomesapkrinhibitorduringhiv1replication
AT burugusamantha pkractivatorpactbecomesapkrinhibitorduringhiv1replication
AT gelinasjeanfrancois pkractivatorpactbecomesapkrinhibitorduringhiv1replication
AT earthornin pkractivatorpactbecomesapkrinhibitorduringhiv1replication
AT sincklucile pkractivatorpactbecomesapkrinhibitorduringhiv1replication
AT routyjeanpierre pkractivatorpactbecomesapkrinhibitorduringhiv1replication
AT moulandandrewj pkractivatorpactbecomesapkrinhibitorduringhiv1replication
AT patelrekhac pkractivatorpactbecomesapkrinhibitorduringhiv1replication
AT gatignolanne pkractivatorpactbecomesapkrinhibitorduringhiv1replication

Ejemplares similares