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Published in: BMC Immunology 1/2014

Open Access 01-12-2014 | Research article

Impact of endobronchial allergen provocation on macrophage phenotype in asthmatics

Authors: Carla Winkler, Lena Witte, Natali Moraw, Conny Faulenbach, Meike Müller, Olaf Holz, Frank Schaumann, Jens M Hohlfeld

Published in: BMC Immunology | Issue 1/2014

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Abstract

Background

The role of M2 polarized macrophages (MΦ) during the allergic airway inflammation has been discussed in various animal models. However, their presence and relevance during the chronic and acute phase of allergic airway inflammation in humans has not been fully elucidated so far. In the present study we phenotypically characterized macrophages with regard to M2 polarization in mice, a human in vitro and a human ex vivo model with primary lung cells after endobronchial provocation.

Results

Macrophages remained polarized beyond clearance of the acute allergic airway inflammation in mice. Alveolar macrophages of asthmatics revealed increased mRNA expression of CCL13, CCL17 and CLEC10A in response to allergen challenge as well as increased surface expression of CD86. Further, mRNA expression of CCL13, CCL17, and CLEC10A was increased in asthmatics at baseline compared to healthy subjects. The mRNA expression of CCL17 and CLEC10A correlated significantly with the degree of eosinophilia (each P < .01). Furthermore, macrophages from asthmatics released significant amounts of CCL17 protein in vitro which was also found increased in BAL fluid after allergen provocation.

Conclusions

This study supports previous findings of M2 macrophage polarization in asthmatic subjects during the acute course of the allergic inflammation and provides evidence for their contribution to the Th2 inflammation.
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Metadata
Title
Impact of endobronchial allergen provocation on macrophage phenotype in asthmatics
Authors
Carla Winkler
Lena Witte
Natali Moraw
Conny Faulenbach
Meike Müller
Olaf Holz
Frank Schaumann
Jens M Hohlfeld
Publication date
01-12-2014
Publisher
BioMed Central
Published in
BMC Immunology / Issue 1/2014
Electronic ISSN: 1471-2172
DOI
https://doi.org/10.1186/1471-2172-15-12

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