Fc gamma receptor IIa suppresses type I and III interferon production by human myeloid immune cells

Type I and type III interferons (IFNs) are fundamental for antiviral immunity, but prolonged expression is also detrimental to the host. Therefore, upon viral infection high levels of type I and III IFNs are followed by a strong and rapid decline. However, the mechanisms responsible for this suppres...

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Autores principales: Newling, Melissa, Hoepel, Willianne, Vogelpoel, Lisa T.C., Heineke, Marieke H., van Burgsteden, Johan A., Taanman‐Kueter, Esther W.M., Eggink, Dirk, Kuijpers, Taco W., Beaumont, Tim, van Egmond, Marjolein, Kapsenberg, Martien L., Baeten, Dominique L.P., den Dunnen, Jeroen, de Jong, Esther C.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: John Wiley and Sons Inc. 2018
Materias:
Innate immunity
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6282563/
https://www.ncbi.nlm.nih.gov/pubmed/30184252
http://dx.doi.org/10.1002/eji.201847615
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author Newling, Melissa
Hoepel, Willianne
Vogelpoel, Lisa T.C.
Heineke, Marieke H.
van Burgsteden, Johan A.
Taanman‐Kueter, Esther W.M.
Eggink, Dirk
Kuijpers, Taco W.
Beaumont, Tim
van Egmond, Marjolein
Kapsenberg, Martien L.
Baeten, Dominique L.P.
den Dunnen, Jeroen
de Jong, Esther C.
author_facet Newling, Melissa
Hoepel, Willianne
Vogelpoel, Lisa T.C.
Heineke, Marieke H.
van Burgsteden, Johan A.
Taanman‐Kueter, Esther W.M.
Eggink, Dirk
Kuijpers, Taco W.
Beaumont, Tim
van Egmond, Marjolein
Kapsenberg, Martien L.
Baeten, Dominique L.P.
den Dunnen, Jeroen
de Jong, Esther C.
author_sort Newling, Melissa
collection PubMed
description Type I and type III interferons (IFNs) are fundamental for antiviral immunity, but prolonged expression is also detrimental to the host. Therefore, upon viral infection high levels of type I and III IFNs are followed by a strong and rapid decline. However, the mechanisms responsible for this suppression are still largely unknown. Here, we show that IgG opsonization of model viruses influenza and respiratory syncytial virus (RSV) strongly and selectively suppressed type I and III IFN production by various human antigen‐presenting cells. This suppression was induced by selective inhibition of TLR, RIG‐I‐like receptor, and STING‐dependent type I and III IFN gene transcription. Surprisingly, type I and III IFN suppression was mediated by Syk and PI3K independent inhibitory signaling via FcγRIIa, thereby identifying a novel non‐canonical FcγRIIa pathway in myeloid cells. Together, these results indicate that IgG opsonization of viruses functions as a novel negative feedback mechanism in humans, which may play a role in the selective suppression of type I and III IFN responses during the late‐phase of viral infections. In addition, activation of this pathway may be used as a tool to limit type I IFN‐associated pathology.
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spelling pubmed-62825632018-12-11 Fc gamma receptor IIa suppresses type I and III interferon production by human myeloid immune cells Newling, Melissa Hoepel, Willianne Vogelpoel, Lisa T.C. Heineke, Marieke H. van Burgsteden, Johan A. Taanman‐Kueter, Esther W.M. Eggink, Dirk Kuijpers, Taco W. Beaumont, Tim van Egmond, Marjolein Kapsenberg, Martien L. Baeten, Dominique L.P. den Dunnen, Jeroen de Jong, Esther C. Eur J Immunol Innate immunity Type I and type III interferons (IFNs) are fundamental for antiviral immunity, but prolonged expression is also detrimental to the host. Therefore, upon viral infection high levels of type I and III IFNs are followed by a strong and rapid decline. However, the mechanisms responsible for this suppression are still largely unknown. Here, we show that IgG opsonization of model viruses influenza and respiratory syncytial virus (RSV) strongly and selectively suppressed type I and III IFN production by various human antigen‐presenting cells. This suppression was induced by selective inhibition of TLR, RIG‐I‐like receptor, and STING‐dependent type I and III IFN gene transcription. Surprisingly, type I and III IFN suppression was mediated by Syk and PI3K independent inhibitory signaling via FcγRIIa, thereby identifying a novel non‐canonical FcγRIIa pathway in myeloid cells. Together, these results indicate that IgG opsonization of viruses functions as a novel negative feedback mechanism in humans, which may play a role in the selective suppression of type I and III IFN responses during the late‐phase of viral infections. In addition, activation of this pathway may be used as a tool to limit type I IFN‐associated pathology. John Wiley and Sons Inc. 2018-09-14 2018-11 /pmc/articles/PMC6282563/ /pubmed/30184252 http://dx.doi.org/10.1002/eji.201847615 Text en © 2018 The Authors. European Journal of Immunology published by WILEY‐VCH Verlag GmbH & Co. KGaA, Weinheim. This is an open access article under the terms of the http://creativecommons.org/licenses/by/4.0/ License, which permits use, distribution and reproduction in any medium, provided the original work is properly cited.
spellingShingle Innate immunity
Newling, Melissa
Hoepel, Willianne
Vogelpoel, Lisa T.C.
Heineke, Marieke H.
van Burgsteden, Johan A.
Taanman‐Kueter, Esther W.M.
Eggink, Dirk
Kuijpers, Taco W.
Beaumont, Tim
van Egmond, Marjolein
Kapsenberg, Martien L.
Baeten, Dominique L.P.
den Dunnen, Jeroen
de Jong, Esther C.
Fc gamma receptor IIa suppresses type I and III interferon production by human myeloid immune cells
title Fc gamma receptor IIa suppresses type I and III interferon production by human myeloid immune cells
title_full Fc gamma receptor IIa suppresses type I and III interferon production by human myeloid immune cells
title_fullStr Fc gamma receptor IIa suppresses type I and III interferon production by human myeloid immune cells
title_full_unstemmed Fc gamma receptor IIa suppresses type I and III interferon production by human myeloid immune cells
title_short Fc gamma receptor IIa suppresses type I and III interferon production by human myeloid immune cells
title_sort fc gamma receptor iia suppresses type i and iii interferon production by human myeloid immune cells
topic Innate immunity
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6282563/
https://www.ncbi.nlm.nih.gov/pubmed/30184252
http://dx.doi.org/10.1002/eji.201847615
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