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Timed Action of IL-27 Protects from Immunopathology while Preserving Defense in Influenza

Infection with influenza virus can result in massive pulmonary infiltration and potentially fatal immunopathology. Understanding the endogenous mechanisms that control immunopathology could provide a key to novel adjunct therapies for this disease. Here we show that the cytokine IL-27 plays a crucia...

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Autores principales: Liu, Francesca Diane M., Kenngott, Elisabeth E., Schröter, Micha F., Kühl, Anja, Jennrich, Silke, Watzlawick, Ralf, Hoffmann, Ute, Wolff, Thorsten, Norley, Stephen, Scheffold, Alexander, Stumhofer, Jason S., Saris, Christiaan J. M., Schwab, Jan M., Hunter, Christopher A., Debes, Gudrun F., Hamann, Alf
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2014
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4014457/
https://www.ncbi.nlm.nih.gov/pubmed/24809349
http://dx.doi.org/10.1371/journal.ppat.1004110
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author Liu, Francesca Diane M.
Kenngott, Elisabeth E.
Schröter, Micha F.
Kühl, Anja
Jennrich, Silke
Watzlawick, Ralf
Hoffmann, Ute
Wolff, Thorsten
Norley, Stephen
Scheffold, Alexander
Stumhofer, Jason S.
Saris, Christiaan J. M.
Schwab, Jan M.
Hunter, Christopher A.
Debes, Gudrun F.
Hamann, Alf
author_facet Liu, Francesca Diane M.
Kenngott, Elisabeth E.
Schröter, Micha F.
Kühl, Anja
Jennrich, Silke
Watzlawick, Ralf
Hoffmann, Ute
Wolff, Thorsten
Norley, Stephen
Scheffold, Alexander
Stumhofer, Jason S.
Saris, Christiaan J. M.
Schwab, Jan M.
Hunter, Christopher A.
Debes, Gudrun F.
Hamann, Alf
author_sort Liu, Francesca Diane M.
collection PubMed
description Infection with influenza virus can result in massive pulmonary infiltration and potentially fatal immunopathology. Understanding the endogenous mechanisms that control immunopathology could provide a key to novel adjunct therapies for this disease. Here we show that the cytokine IL-27 plays a crucial role in protection from exaggerated inflammation during influenza virus infection. Using Il-27ra (−/−) mice, IL-27 was found to limit immunopathology, neutrophil accumulation, and dampened T(H)1 or T(H)17 responses via IL-10–dependent and -independent pathways. Accordingly, the absence of IL-27 signals resulted in a more severe disease course and in diminished survival without impacting viral loads. Consistent with the delayed expression of endogenous Il-27p28 during influenza, systemic treatment with recombinant IL-27 starting at the peak of virus load resulted in a major amelioration of lung pathology, strongly reduced leukocyte infiltration and improved survival without affecting viral clearance. In contrast, early application of IL-27 impaired virus clearance and worsened disease. These findings demonstrate the importance of IL-27 for the physiological control of immunopathology and the potential value of well-timed IL-27 application to treat life-threatening inflammation during lung infection.
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spelling pubmed-40144572014-05-14 Timed Action of IL-27 Protects from Immunopathology while Preserving Defense in Influenza Liu, Francesca Diane M. Kenngott, Elisabeth E. Schröter, Micha F. Kühl, Anja Jennrich, Silke Watzlawick, Ralf Hoffmann, Ute Wolff, Thorsten Norley, Stephen Scheffold, Alexander Stumhofer, Jason S. Saris, Christiaan J. M. Schwab, Jan M. Hunter, Christopher A. Debes, Gudrun F. Hamann, Alf PLoS Pathog Research Article Infection with influenza virus can result in massive pulmonary infiltration and potentially fatal immunopathology. Understanding the endogenous mechanisms that control immunopathology could provide a key to novel adjunct therapies for this disease. Here we show that the cytokine IL-27 plays a crucial role in protection from exaggerated inflammation during influenza virus infection. Using Il-27ra (−/−) mice, IL-27 was found to limit immunopathology, neutrophil accumulation, and dampened T(H)1 or T(H)17 responses via IL-10–dependent and -independent pathways. Accordingly, the absence of IL-27 signals resulted in a more severe disease course and in diminished survival without impacting viral loads. Consistent with the delayed expression of endogenous Il-27p28 during influenza, systemic treatment with recombinant IL-27 starting at the peak of virus load resulted in a major amelioration of lung pathology, strongly reduced leukocyte infiltration and improved survival without affecting viral clearance. In contrast, early application of IL-27 impaired virus clearance and worsened disease. These findings demonstrate the importance of IL-27 for the physiological control of immunopathology and the potential value of well-timed IL-27 application to treat life-threatening inflammation during lung infection. Public Library of Science 2014-05-08 /pmc/articles/PMC4014457/ /pubmed/24809349 http://dx.doi.org/10.1371/journal.ppat.1004110 Text en © 2014 Liu 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
Liu, Francesca Diane M.
Kenngott, Elisabeth E.
Schröter, Micha F.
Kühl, Anja
Jennrich, Silke
Watzlawick, Ralf
Hoffmann, Ute
Wolff, Thorsten
Norley, Stephen
Scheffold, Alexander
Stumhofer, Jason S.
Saris, Christiaan J. M.
Schwab, Jan M.
Hunter, Christopher A.
Debes, Gudrun F.
Hamann, Alf
Timed Action of IL-27 Protects from Immunopathology while Preserving Defense in Influenza
title Timed Action of IL-27 Protects from Immunopathology while Preserving Defense in Influenza
title_full Timed Action of IL-27 Protects from Immunopathology while Preserving Defense in Influenza
title_fullStr Timed Action of IL-27 Protects from Immunopathology while Preserving Defense in Influenza
title_full_unstemmed Timed Action of IL-27 Protects from Immunopathology while Preserving Defense in Influenza
title_short Timed Action of IL-27 Protects from Immunopathology while Preserving Defense in Influenza
title_sort timed action of il-27 protects from immunopathology while preserving defense in influenza
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4014457/
https://www.ncbi.nlm.nih.gov/pubmed/24809349
http://dx.doi.org/10.1371/journal.ppat.1004110
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