RRC ID 88540
Author Miyagawa F, Ozato K, Tagaya Y, Asada H.
Title Type I IFN Derived from Ly6Chi Monocytes Suppresses Type 2 Inflammation in a Murine Model of Atopic Dermatitis.
Journal J Invest Dermatol
Abstract The roles of innate immune cells, including eosinophils, basophils, and group 2 innate lymphoid cells, in atopic dermatitis (AD) have been well-documented, whereas that of monocytes, another component of the innate immunity, remains rather poorly understood, thus necessitating the topic of this study. In addition, cytokines and cellular pathways needed for the resolution of type 2 inflammation in AD need further investigation. Using a murine AD model, we report here that (i) Ly6Chi monocytes were rapidly recruited to the AD lesion in a CCR2-dependent manner, blockade of which exacerbated AD; (ii) type I IFN production is profoundly involved in this suppression because the blockade of it by genetic depletion or antibody neutralization exacerbated AD; and (iii) Ly6Chi monocytes operate through the production of type I IFN because Ly6Chi monocytes from Irf7-null mice, which lack type I IFN production, failed to rescue Ccr2-/- mice from severe AD upon adoptive transfer. In addition, in vitro studies demonstrated type I IFN suppressed basophil expansion from bone marrow progenitor cells and survival of mature basophils. Collectively, our work suggests that Ly6Chi monocytes are the first and dominant inflammatory cells reaching AD lesions that negatively regulate type 2 inflammation through the production of type I IFN.
Volume 144(3)
Pages 520-530.e2
Published 2024-3-1
DOI 10.1016/j.jid.2023.08.022
PII S0022-202X(23)02588-5
PMID 37739337
MeSH Animals Antigens, Ly / metabolism Dermatitis, Atopic* / pathology Disease Models, Animal Immunity, Innate Inflammation / pathology Lymphocytes / metabolism Mice Mice, Inbred C57BL Mice, Knockout Monocytes*
Resource
Mice RBRC01420