Dendritic cell-bound IgE functions to restrain allergic inflammation at mucosal sites

Antigen-mediated crosslinking of Immunoglobulin E (IgE) bound to mast cells/basophils via FcεRI, the high affinity IgE Fc-receptor, is a well-known trigger of allergy. In humans, but not mice, dendritic cells (DCs) also express FcεRI that is constitutively occupied with IgE. In contrast to mast cell...

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Autores principales: Platzer, Barbara, Baker, Kristi, Vera, Miguel Pinilla, Singer, Kathleen, Panduro, Marisella, Lexmond, Willem S., Turner, Devin, Vargas, Sara O., Kinet, Jean-Pierre, Maurer, Dieter, Baron, Rebecca M., Blumberg, Richard S., Fiebiger, Edda
Formato: Online Artículo Texto
Lenguaje:English
Publicado: 2014
Materias:
Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4363306/
https://www.ncbi.nlm.nih.gov/pubmed/25227985
http://dx.doi.org/10.1038/mi.2014.85
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author Platzer, Barbara
Baker, Kristi
Vera, Miguel Pinilla
Singer, Kathleen
Panduro, Marisella
Lexmond, Willem S.
Turner, Devin
Vargas, Sara O.
Kinet, Jean-Pierre
Maurer, Dieter
Baron, Rebecca M.
Blumberg, Richard S.
Fiebiger, Edda
author_facet Platzer, Barbara
Baker, Kristi
Vera, Miguel Pinilla
Singer, Kathleen
Panduro, Marisella
Lexmond, Willem S.
Turner, Devin
Vargas, Sara O.
Kinet, Jean-Pierre
Maurer, Dieter
Baron, Rebecca M.
Blumberg, Richard S.
Fiebiger, Edda
author_sort Platzer, Barbara
collection PubMed
description Antigen-mediated crosslinking of Immunoglobulin E (IgE) bound to mast cells/basophils via FcεRI, the high affinity IgE Fc-receptor, is a well-known trigger of allergy. In humans, but not mice, dendritic cells (DCs) also express FcεRI that is constitutively occupied with IgE. In contrast to mast cells/basophils, the consequences of IgE/FcεRI signals for DC function remain poorly understood. We show that humanized mice that express FcεRI on DCs carry IgE like non-allergic humans and do not develop spontaneous allergies. Antigen-specific IgE/FcεRI crosslinking fails to induce maturation or production of inflammatory mediators in human DCs and FcεRI-humanized DCs. Furthermore, conferring expression of FcεRI to DCs decreases the severity of food allergy and asthma in disease-relevant models suggesting anti-inflammatory IgE/FcεRI signals. Consistent with the improved clinical parameters in vivo, antigen-specific IgE/FcεRI crosslinking on papain or LPS-stimulated DCs inhibits the production of pro-inflammatory cytokines and chemokines. Migration assays confirm that the IgE-dependent decrease in cytokine production results in diminished recruitment of mast cell progenitors; providing a mechanistic explanation for the reduced mast cell-dependent allergic phenotype observed in FcεRI-humanized mice. Our study demonstrates a novel immune regulatory function of IgE and proposes that DC-intrinsic IgE signals serve as a feedback mechanism to restrain allergic tissue inflammation.
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spelling pubmed-43633062015-11-01 Dendritic cell-bound IgE functions to restrain allergic inflammation at mucosal sites Platzer, Barbara Baker, Kristi Vera, Miguel Pinilla Singer, Kathleen Panduro, Marisella Lexmond, Willem S. Turner, Devin Vargas, Sara O. Kinet, Jean-Pierre Maurer, Dieter Baron, Rebecca M. Blumberg, Richard S. Fiebiger, Edda Mucosal Immunol Article Antigen-mediated crosslinking of Immunoglobulin E (IgE) bound to mast cells/basophils via FcεRI, the high affinity IgE Fc-receptor, is a well-known trigger of allergy. In humans, but not mice, dendritic cells (DCs) also express FcεRI that is constitutively occupied with IgE. In contrast to mast cells/basophils, the consequences of IgE/FcεRI signals for DC function remain poorly understood. We show that humanized mice that express FcεRI on DCs carry IgE like non-allergic humans and do not develop spontaneous allergies. Antigen-specific IgE/FcεRI crosslinking fails to induce maturation or production of inflammatory mediators in human DCs and FcεRI-humanized DCs. Furthermore, conferring expression of FcεRI to DCs decreases the severity of food allergy and asthma in disease-relevant models suggesting anti-inflammatory IgE/FcεRI signals. Consistent with the improved clinical parameters in vivo, antigen-specific IgE/FcεRI crosslinking on papain or LPS-stimulated DCs inhibits the production of pro-inflammatory cytokines and chemokines. Migration assays confirm that the IgE-dependent decrease in cytokine production results in diminished recruitment of mast cell progenitors; providing a mechanistic explanation for the reduced mast cell-dependent allergic phenotype observed in FcεRI-humanized mice. Our study demonstrates a novel immune regulatory function of IgE and proposes that DC-intrinsic IgE signals serve as a feedback mechanism to restrain allergic tissue inflammation. 2014-09-17 2015-05 /pmc/articles/PMC4363306/ /pubmed/25227985 http://dx.doi.org/10.1038/mi.2014.85 Text en http://www.nature.com/authors/editorial_policies/license.html#terms Users may view, print, copy, and download text and data-mine the content in such documents, for the purposes of academic research, subject always to the full Conditions of use:http://www.nature.com/authors/editorial_policies/license.html#terms
spellingShingle Article
Platzer, Barbara
Baker, Kristi
Vera, Miguel Pinilla
Singer, Kathleen
Panduro, Marisella
Lexmond, Willem S.
Turner, Devin
Vargas, Sara O.
Kinet, Jean-Pierre
Maurer, Dieter
Baron, Rebecca M.
Blumberg, Richard S.
Fiebiger, Edda
Dendritic cell-bound IgE functions to restrain allergic inflammation at mucosal sites
title Dendritic cell-bound IgE functions to restrain allergic inflammation at mucosal sites
title_full Dendritic cell-bound IgE functions to restrain allergic inflammation at mucosal sites
title_fullStr Dendritic cell-bound IgE functions to restrain allergic inflammation at mucosal sites
title_full_unstemmed Dendritic cell-bound IgE functions to restrain allergic inflammation at mucosal sites
title_short Dendritic cell-bound IgE functions to restrain allergic inflammation at mucosal sites
title_sort dendritic cell-bound ige functions to restrain allergic inflammation at mucosal sites
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4363306/
https://www.ncbi.nlm.nih.gov/pubmed/25227985
http://dx.doi.org/10.1038/mi.2014.85
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