Details der Publikation - Allergic airway inflammation induces upregulation of the expression of IL-23R by macrophages and not in CD3 + T cells and $ CD11c^{+} $F4/$ 80^{−} $ dendritic cells of the lung

Allergic airway inflammation induces upregulation of the expression of IL-23R by macrophages and not in CD3 + T cells and $ CD11c^{+} $F4/$ 80^{−} $ dendritic cells of the lung

Abstract Interleukin 23 and the interleukin 23 receptor (IL-23-IL23R) are described as the major enhancing factors for Interleukin 17 (IL-17) in allergic airway inflammation. IL-17 is considered to induce neutrophilic inflammation in the lung, which is often observed in severe, steroid-resistant asthma-phenotypes. For that reason, understanding of IL-23 and IL-17 axis is very important for future therapy strategies, targeting neutrophil pathway of bronchial asthma. This study aimed to investigate the distribution and expression of IL-23R under physiological and inflammatory conditions. Therefore, a house dust mite (HDM) model of allergic airway inflammation was performed by treating mice with HDM intranasally. Immunofluorescence staining with panel of antibodies was performed in lung tissues to examine the macrophage, dendritic cell, and T cell subpopulations. The allergic airway inflammation was quantified by histopathological analysis, ELISA measurements, and airway function. HDM-treated mice exhibited a significant allergic airway inflammation including higher amounts of $ NE^{+} $ cells in lung parenchyma. We found only a small amount of IL-23R positives, out of total $ CD3^{+} $T cells, and no upregulation in HDM-treated animals. In contrast, the populations of F4/$ 80^{+} $ macrophages and $ CD11c^{+} $F4/$ 80^{−} $ dendritic cells (DCs) with IL-23R expression were found to be higher. But HDM treatment leads to a significant increase of IL-$ 23R^{+} $ macrophages, only. IL-23R was expressed by every examined macrophage subpopulation, whereas only Mϕ1 and hybrids between Mϕ1 and Mϕ2 phenotype and not Mϕ2 were found to upregulate IL-23R. Co-localization of IL-23R and IL-17 was only observed in F4/$ 80^{+} $ macrophages, suggesting F4/$ 80^{+} $ macrophages express IL-23R along with IL-17 in lung tissue. The study revealed that macrophages involving the IL-23 and IL-17 pathway may provide a potential interesting therapeutic target in neutrophilic bronchial asthma..

Medienart:	E-Artikel

Erscheinungsjahr:	2022
Erschienen:	2022

Enthalten in:	Zur Gesamtaufnahme - volume:389
Enthalten in:	Cell & tissue research - 389(2022), 1 vom: 27. Apr., Seite 85-98

Sprache:	Englisch

Beteiligte Personen:	Leitner, Maximilian [VerfasserIn] Heck, Sebastian [VerfasserIn] Nguyen, Kenny [VerfasserIn] Nguyen, Phu Quyen [VerfasserIn] Harfoush, Shaza [VerfasserIn] Rosenkranz, Eva [VerfasserIn] Bals, Robert [VerfasserIn] Dinh, Quoc Thai [VerfasserIn]

Links:	Volltext [kostenfrei]

BKL:	42.15$jZellbiologie
Themen:	Airway neutrophilia Allergic airway inflammation IL-23 IL-23R Macrophages

RVK:	RVK Klassifikation ELIB24

Anmerkungen:	© The Author(s) 2022

doi:	10.1007/s00441-021-03538-0

funding:
Förderinstitution / Projekttitel:

PPN (Katalog-ID):	OLC2130914896

Internformat


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520			\|a Abstract Interleukin 23 and the interleukin 23 receptor (IL-23-IL23R) are described as the major enhancing factors for Interleukin 17 (IL-17) in allergic airway inflammation. IL-17 is considered to induce neutrophilic inflammation in the lung, which is often observed in severe, steroid-resistant asthma-phenotypes. For that reason, understanding of IL-23 and IL-17 axis is very important for future therapy strategies, targeting neutrophil pathway of bronchial asthma. This study aimed to investigate the distribution and expression of IL-23R under physiological and inflammatory conditions. Therefore, a house dust mite (HDM) model of allergic airway inflammation was performed by treating mice with HDM intranasally. Immunofluorescence staining with panel of antibodies was performed in lung tissues to examine the macrophage, dendritic cell, and T cell subpopulations. The allergic airway inflammation was quantified by histopathological analysis, ELISA measurements, and airway function. HDM-treated mice exhibited a significant allergic airway inflammation including higher amounts of $ NE^{+} $ cells in lung parenchyma. We found only a small amount of IL-23R positives, out of total $ CD3^{+} $T cells, and no upregulation in HDM-treated animals. In contrast, the populations of F4/$ 80^{+} $ macrophages and $ CD11c^{+} $F4/$ 80^{−} $ dendritic cells (DCs) with IL-23R expression were found to be higher. But HDM treatment leads to a significant increase of IL-$ 23R^{+} $ macrophages, only. IL-23R was expressed by every examined macrophage subpopulation, whereas only Mϕ1 and hybrids between Mϕ1 and Mϕ2 phenotype and not Mϕ2 were found to upregulate IL-23R. Co-localization of IL-23R and IL-17 was only observed in F4/$ 80^{+} $ macrophages, suggesting F4/$ 80^{+} $ macrophages express IL-23R along with IL-17 in lung tissue. The study revealed that macrophages involving the IL-23 and IL-17 pathway may provide a potential interesting therapeutic target in neutrophilic bronchial asthma.
650		4	\|a IL-23
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650		4	\|a Allergic airway inflammation
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700	1		\|a Heck, Sebastian \|4 aut
700	1		\|a Nguyen, Kenny \|4 aut
700	1		\|a Nguyen, Phu Quyen \|4 aut
700	1		\|a Harfoush, Shaza \|4 aut
700	1		\|a Rosenkranz, Eva \|4 aut
700	1		\|a Bals, Robert \|4 aut
700	1		\|a Dinh, Quoc Thai \|4 aut
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Allergic airway inflammation induces upregulation of the expression of IL-23R by macrophages and not in CD3 + T cells and $ CD11c^{+} $F4/$ 80^{−} $ dendritic cells of the lung

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