| Literature DB >> 29474945 |
Nick Vandeghinste1, Jürgen Klattig2, Catherine Jagerschmidt3, Stéphanie Lavazais3, Florence Marsais3, Jan D Haas2, Marielle Auberval3, Felix Lauffer4, Tara Moran5, Mate Ongenaert6, Maarten Van Balen6, Sonia Dupont3, Liên Lepescheux3, Teresa Garcia3, Stefan Härtle2, Kilian Eyerich4, Padraic G Fallon5, Reginald Brys6, Stefan Steidl2.
Abstract
IL-17C is a functionally distinct member of the IL-17 family that was believed to play a role in the pathogenesis of psoriasis. Here we confirmed that IL-17C is involved in psoriasis and explored potential roles for IL-17C in atopic dermatitis (AD). An anti-IL-17C antibody, MOR106, was generated that potently and selectively binds to human and mouse IL-17C, thereby inhibiting the binding of IL-17C to its IL-17RE receptor. The antibody inhibited cutaneous inflammation in an IL-23-induced psoriatic-like skin inflammation model. In lesional skin of patients with AD, IL-17C expression levels were increased and localized to keratinocytes and infiltrating immune cells. To determine the contribution of IL-17C to AD pathogenesis, MOR106 was tested in two distinct in vivo models. In the calcipotriol-induced AD model, ear skin inflammation, TSLP, and IL-33 protein production in ears was suppressed by MOR106. Consistently, in the flaky tail strain mouse model, spontaneous development of AD-like skin inflammation was reduced by MOR106. Moreover, serum IgE levels, number of mast cells in skin and T helper type 2-related cytokines IL-4 and CCL17 in serum were all reduced. Overall, our results indicate that IL-17C is a central mediator of skin inflammation beyond psoriasis and is relevant in particular in AD.Entities:
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Year: 2018 PMID: 29474945 DOI: 10.1016/j.jid.2018.01.036
Source DB: PubMed Journal: J Invest Dermatol ISSN: 0022-202X Impact factor: 8.551