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IL-25 enhances TH17 cell–mediated contact dermatitis by promoting IL-1? production by dermal dendritic cells - 06/11/18

Doi : 10.1016/j.jaci.2017.12.1007 
Hajime Suto, MD, PhD a, , Aya Nambu, PhD b, , Hideaki Morita, MD, PhD c, , Sachiko Yamaguchi, MS b, Takafumi Numata, MD, PhD b, Takamichi Yoshizaki, MD b, Eri Shimura, PhD a, b, Ken Arae, PhD c, d, Yousuke Asada, MD, PhD e, Kenichiro Motomura, MD, PhD c, Mari Kaneko f, g, Takaya Abe, PhD g, Akira Matsuda, MD, PhD e, Yoichiro Iwakura, DSc h, Ko Okumura, MD, PhD a, Hirohisa Saito, MD, PhD c, Kenji Matsumoto, MD, PhD c, Katsuko Sudo, PhD i, Susumu Nakae, PhD b, j,
a Atopy Research Center, Juntendo University, Tokyo, Japan 
e Department of Ophthalmology, Juntendo University, Tokyo, Japan 
b Laboratory of Systems Biology, Center for Experimental Medicine and Systems Biology, Institute of Medical Science, University of Tokyo, Tokyo, Japan 
c Department of Allergy and Clinical Immunology, National Research Institute for Child Health and Development, Tokyo, Japan 
d Department of Immunology, Faculty of Health Science, Kyorin University, Tokyo, Japan 
f Animal Resource Development Unit, RIKEN Center for Life Science Technologies, Kobe, Japan 
g Genetic Engineering Team, RIKEN Center for Life Science Technologies, Kobe, Japan 
h Center for Experimental Animal Models, Institute for Biomedical Sciences, Tokyo University of Science, Chiba, Japan 
i Animal Research Center, Tokyo Medical University, Tokyo, Japan 
j Precursory Research for Embryonic Science and Technology, Japan Science and Technology Agency, Saitama, Japan 

Corresponding author: Susumu Nakae, PhD, Laboratory of Systems Biology, Center for Experimental Medicine and Systems Biology, Institute of Medical Science, University of Tokyo, 4-6-1 Shirokanedai, Minato, Tokyo, 108-8639, Japan.Laboratory of Systems BiologyCenter for Experimental Medicine and Systems BiologyInstitute of Medical ScienceUniversity of Tokyo4-6-1 Shirokanedai, MinatoTokyo108-8639Japan

Abstract

Background

In addition to thymic stromal lymphopoietin and IL-33, IL-25 is known to induce TH2 cytokine production by various cell types, including TH2 cells, TH9 cells, invariant natural killer T cells, and group 2 innate lymphoid cells, involved in TH2-type immune responses. Because both TH2-type and TH17-type cells/cytokines are crucial for contact hypersensitivity (CHS), IL-25 can contribute to this by enhancing TH2-type immune responses. However, the precise role of IL-25 in the pathogenesis of fluorescein isothiocyanate–induced CHS is poorly understood.

Objective

We investigated the contribution of IL-25 to CHS using Il25−/− mice.

Methods

CHS was evaluated by means of measurement of ear skin thickness in mice after fluorescein isothiocyanate painting. Skin dendritic cell (DC) migration, hapten-specific TH cell differentiation, and detection of IL-1β–producing cells were determined by using flow cytometry, ELISA, and immunohistochemistry, respectively.

Results

In contrast to thymic stromal lymphopoietin, we found that IL-25 was not essential for skin DC migration or hapten-specific TH cell differentiation in the sensitization phase of CHS. Unexpectedly, mast cell– and non–immune cell–derived IL-25 was important for hapten-specific TH17 cell–mediated rather than TH2 cell–mediated inflammation in the elicitation phase of CHS by enhancing TH17-related, but not TH2-related, cytokines in the skin. In particular, IL-1β produced by dermal DCs in response to IL-25 was crucial for hapten-specific TH17 cell activation, contributing to induction of local inflammation in the elicitation phase of CHS.

Conclusion

Our results identify a novel IL-25 inflammatory pathway involved in induction of TH17 cell–mediated, but not TH2 cell–mediated, CHS. IL-25 neutralization can be a potential approach for treatment of CHS.

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Graphical abstract




Le texte complet de cet article est disponible en PDF.

Key words : IL-25, IL-33, thymic stromal lymphopoietin, contact hypersensitivity, gene-deficient mice, TH2, TH17

Abbreviations used : BM, BMDC, CHS, DC, DNFB, EPO, FITC, LN, MC, MPO, TSLP, WT


Plan


 Supported by Grants-in-Aid for Young Scientists (A and B; to S.N.); the Program for Improvement of Research Environment for Young Researchers, Special Coordination Funds for Promoting Science and Technology (to S.N.), from the Ministry of Education, Culture, Sports, Science and Technology, Japan; Precursory Research for Embryonic Science and Technology, Japan Science and Technology Agency (to S.N.); a Health Labour Sciences Research Grant from the Ministry of Health, Labour and Welfare, Japan (to H.S., S.N., and K.M.); and a grant from the Japan Chemical Industry Association Long-range Research Initiative (to S.N.).
 Disclosure of potential conflict of interest: H. Morita is employed by the National Research Institute for Child Health and Development. H. Saito received payment for lectures from Shiseido, MSD (Merck Sharp and Dohme), and AstraZeneca. K. Matsumoto is employed by the National Research Institute for Child Health and Development and received payment for lectures from MSD (Merck Sharp and Dohme), Kyorin Pharmaceutical, AstraZeneca, Maruho, Teijin Pharma, and Chugai Pharmaceutical. The rest of the authors declare that they have no relevant conflicts of interest.


© 2018  American Academy of Allergy, Asthma & Immunology. Publié par Elsevier Masson SAS. Tous droits réservés.
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