Impairment of Immunoproteasome Function by β5i/LMP7 Subunit Deficiency Results in Severe Enterovirus Myocarditis

Proteasomes recognize and degrade poly-ubiquitinylated proteins. In infectious disease, cells activated by interferons (IFNs) express three unique catalytic subunits β1i/LMP2, β2i/MECL-1 and β5i/LMP7 forming an alternative proteasome isoform, the immunoproteasome (IP). The in vivo function of IPs in...

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Autores principales: Opitz, Elisa, Koch, Annett, Klingel, Karin, Schmidt, Frank, Prokop, Stefan, Rahnefeld, Anna, Sauter, Martina, Heppner, Frank L., Völker, Uwe, Kandolf, Reinhard, Kuckelkorn, Ulrike, Stangl, Karl, Krüger, Elke, Kloetzel, Peter M., Voigt, Antje
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2011
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3164653/
https://www.ncbi.nlm.nih.gov/pubmed/21909276
http://dx.doi.org/10.1371/journal.ppat.1002233
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author Opitz, Elisa
Koch, Annett
Klingel, Karin
Schmidt, Frank
Prokop, Stefan
Rahnefeld, Anna
Sauter, Martina
Heppner, Frank L.
Völker, Uwe
Kandolf, Reinhard
Kuckelkorn, Ulrike
Stangl, Karl
Krüger, Elke
Kloetzel, Peter M.
Voigt, Antje
author_facet Opitz, Elisa
Koch, Annett
Klingel, Karin
Schmidt, Frank
Prokop, Stefan
Rahnefeld, Anna
Sauter, Martina
Heppner, Frank L.
Völker, Uwe
Kandolf, Reinhard
Kuckelkorn, Ulrike
Stangl, Karl
Krüger, Elke
Kloetzel, Peter M.
Voigt, Antje
author_sort Opitz, Elisa
collection PubMed
description Proteasomes recognize and degrade poly-ubiquitinylated proteins. In infectious disease, cells activated by interferons (IFNs) express three unique catalytic subunits β1i/LMP2, β2i/MECL-1 and β5i/LMP7 forming an alternative proteasome isoform, the immunoproteasome (IP). The in vivo function of IPs in pathogen-induced inflammation is still a matter of controversy. IPs were mainly associated with MHC class I antigen processing. However, recent findings pointed to a more general function of IPs in response to cytokine stress. Here, we report on the role of IPs in acute coxsackievirus B3 (CVB3) myocarditis reflecting one of the most common viral disease entities among young people. Despite identical viral load in both control and IP-deficient mice, IP-deficiency was associated with severe acute heart muscle injury reflected by large foci of inflammatory lesions and severe myocardial tissue damage. Exacerbation of acute heart muscle injury in this host was ascribed to disequilibrium in protein homeostasis in viral heart disease as indicated by the detection of increased proteotoxic stress in cytokine-challenged cardiomyocytes and inflammatory cells from IP-deficient mice. In fact, due to IP-dependent removal of poly-ubiquitinylated protein aggregates in the injured myocardium IPs protected CVB3-challenged mice from oxidant-protein damage. Impaired NFκB activation in IP-deficient cardiomyocytes and inflammatory cells and proteotoxic stress in combination with severe inflammation in CVB3-challenged hearts from IP-deficient mice potentiated apoptotic cell death in this host, thus exacerbating acute tissue damage. Adoptive T cell transfer studies in IP-deficient mice are in agreement with data pointing towards an effective CD8 T cell immune. This study therefore demonstrates that IP formation primarily protects the target organ of CVB3 infection from excessive inflammatory tissue damage in a virus-induced proinflammatory cytokine milieu.
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spelling pubmed-31646532011-09-09 Impairment of Immunoproteasome Function by β5i/LMP7 Subunit Deficiency Results in Severe Enterovirus Myocarditis Opitz, Elisa Koch, Annett Klingel, Karin Schmidt, Frank Prokop, Stefan Rahnefeld, Anna Sauter, Martina Heppner, Frank L. Völker, Uwe Kandolf, Reinhard Kuckelkorn, Ulrike Stangl, Karl Krüger, Elke Kloetzel, Peter M. Voigt, Antje PLoS Pathog Research Article Proteasomes recognize and degrade poly-ubiquitinylated proteins. In infectious disease, cells activated by interferons (IFNs) express three unique catalytic subunits β1i/LMP2, β2i/MECL-1 and β5i/LMP7 forming an alternative proteasome isoform, the immunoproteasome (IP). The in vivo function of IPs in pathogen-induced inflammation is still a matter of controversy. IPs were mainly associated with MHC class I antigen processing. However, recent findings pointed to a more general function of IPs in response to cytokine stress. Here, we report on the role of IPs in acute coxsackievirus B3 (CVB3) myocarditis reflecting one of the most common viral disease entities among young people. Despite identical viral load in both control and IP-deficient mice, IP-deficiency was associated with severe acute heart muscle injury reflected by large foci of inflammatory lesions and severe myocardial tissue damage. Exacerbation of acute heart muscle injury in this host was ascribed to disequilibrium in protein homeostasis in viral heart disease as indicated by the detection of increased proteotoxic stress in cytokine-challenged cardiomyocytes and inflammatory cells from IP-deficient mice. In fact, due to IP-dependent removal of poly-ubiquitinylated protein aggregates in the injured myocardium IPs protected CVB3-challenged mice from oxidant-protein damage. Impaired NFκB activation in IP-deficient cardiomyocytes and inflammatory cells and proteotoxic stress in combination with severe inflammation in CVB3-challenged hearts from IP-deficient mice potentiated apoptotic cell death in this host, thus exacerbating acute tissue damage. Adoptive T cell transfer studies in IP-deficient mice are in agreement with data pointing towards an effective CD8 T cell immune. This study therefore demonstrates that IP formation primarily protects the target organ of CVB3 infection from excessive inflammatory tissue damage in a virus-induced proinflammatory cytokine milieu. Public Library of Science 2011-09-01 /pmc/articles/PMC3164653/ /pubmed/21909276 http://dx.doi.org/10.1371/journal.ppat.1002233 Text en Opitz et al. http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
spellingShingle Research Article
Opitz, Elisa
Koch, Annett
Klingel, Karin
Schmidt, Frank
Prokop, Stefan
Rahnefeld, Anna
Sauter, Martina
Heppner, Frank L.
Völker, Uwe
Kandolf, Reinhard
Kuckelkorn, Ulrike
Stangl, Karl
Krüger, Elke
Kloetzel, Peter M.
Voigt, Antje
Impairment of Immunoproteasome Function by β5i/LMP7 Subunit Deficiency Results in Severe Enterovirus Myocarditis
title Impairment of Immunoproteasome Function by β5i/LMP7 Subunit Deficiency Results in Severe Enterovirus Myocarditis
title_full Impairment of Immunoproteasome Function by β5i/LMP7 Subunit Deficiency Results in Severe Enterovirus Myocarditis
title_fullStr Impairment of Immunoproteasome Function by β5i/LMP7 Subunit Deficiency Results in Severe Enterovirus Myocarditis
title_full_unstemmed Impairment of Immunoproteasome Function by β5i/LMP7 Subunit Deficiency Results in Severe Enterovirus Myocarditis
title_short Impairment of Immunoproteasome Function by β5i/LMP7 Subunit Deficiency Results in Severe Enterovirus Myocarditis
title_sort impairment of immunoproteasome function by β5i/lmp7 subunit deficiency results in severe enterovirus myocarditis
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3164653/
https://www.ncbi.nlm.nih.gov/pubmed/21909276
http://dx.doi.org/10.1371/journal.ppat.1002233
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