Ets1 suppresses atopic dermatitis by suppressing pathogenic T cell responses
Choong-Gu Lee, … , Zee Yong Park, Sin-Hyeog Im
Choong-Gu Lee, … , Zee Yong Park, Sin-Hyeog Im
Published March 7, 2019
Citation Information: JCI Insight. 2019;4(5):e124202. https://doi.org/10.1172/jci.insight.124202.
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Research Article Immunology

Ets1 suppresses atopic dermatitis by suppressing pathogenic T cell responses

Abstract

Atopic dermatitis (AD) is a complex inflammatory skin disease mediated by immune cells of both adaptive and innate types. Among them, CD4+ Th cells are one of major players of AD pathogenesis. Although the pathogenic role of Th2 cells has been well characterized, Th17/Th22 cells are also implicated in the pathogenesis of AD. However, the molecular mechanisms underlying pathogenic immune responses in AD remain unclear. We sought to investigate how the defect in the AD susceptibility gene, Ets1, is involved in AD pathogenesis in human and mice and its clinical relevance in disease severity by identifying Ets1 target genes and binding partners. Consistent with the decrease in ETS1 levels in severe AD patients and the experimental AD-like skin inflammation model, T cell–specific Ets1-deficient mice (Ets1ΔdLck) developed severe AD-like symptoms with increased pathogenic Th cell responses. A T cell–intrinsic increase of gp130 expression upon Ets1 deficiency promotes the gp130-mediated IL-6 signaling pathway, thereby leading to the development of severe AD-like symptoms. Functional blocking of gp130 by selective inhibitor SC144 ameliorated the disease pathogenesis by reducing pathogenic Th cell responses. Our results reveal a protective role of Ets1 in restricting pathogenic Th cell responses and suggest a potential therapeutic target for AD treatment.

Authors

Choong-Gu Lee, Ho-Keun Kwon, Hyeji Kang, Young Kim, Jong Hee Nam, Young Ho Won, Sunhee Park, Taemook Kim, Keunsoo Kang, Dipayan Rudra, Chang-Duk Jun, Zee Yong Park, Sin-Hyeog Im

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Figure 6

The gp130 inhibitor SC144 suppresses pathophysiology of AD in Ets1ΔdLck mice.

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The gp130 inhibitor SC144 suppresses pathophysiology of AD in Ets1ΔdLck ...
Experimental AD was induced in LMC and Ets1ΔdLck mice. The gp130 inhibitor, SC144, was administered via i.p. routes a week after the initial sensitization (5 times during weekdays for 3 weeks) and continued until the end of experiment. (A) H&E staining of the ear biopsies confirmed the clinical symptoms of AD. (B) Ear thickness during the course of AD was measured. The data are expressed as mean ± SD. ****P ≤ 0.0001 (from day 21–31); 2-way ANOVA. (C and D) Cells from the ear tissues were collected from each group of mice under AD (C) and absolute number and frequency of CD4+ T cells were calculated (D). (E–G) The total IgE (E), HDM allergen-specific IgE (F), and total IgG levels (G) in serum from the mouse groups were measured by ELISA. (H) Intracellular staining of IL-17 and IL-22 by CD4-gated T cells were analyzed. Data represent results from 3 independent experiments. Error bars represent the mean ± SEM. *P ≤ 0.05; **P ≤ 0.005; ***P ≤ 0.0005; ****P ≤ 0.0001; Student’s t test.