Macrophage‐mediated psoriasis can be suppressed by regulatory T lymphocytes

银屑病 免疫学 巨噬细胞 医学 化学 体外 生物化学
作者
Rafael Leite Dantas,Dörthe Masemann,Tanja Schied,Vera Bergmeier,Thomas Vogl,Karin Loser,Bent Brachvogel,Georg Varga,Stephan Ludwig,Viktor Wixler
标识
DOI:10.1002/path.4786
摘要

Abstract We recently described an inducible human TNF transgenic mouse line ( ihTNFtg ) that develops psoriasis‐like arthritis after doxycycline stimulation and analysed the pathogenesis of arthritis in detail. Here, we show that the skin phenotype of these mice is characterized by hyperproliferation and aberrant activation of keratinocytes, induction of pro‐inflammatory cytokines, and infiltration with Th1 and Treg lymphocytes, particularly with macrophage infiltration into lesional skin, thus pointing to a psoriasis‐like phenotype. To reveal the contribution of T cells and macrophages to the development of TNF ‐mediated psoriasis, ihTNFtg mice were crossbred into RAG1 KO mice lacking mature T and B cells. Surprisingly, the psoriatic phenotype in the double mutants was not reduced; rather, it was enhanced. The skin showed significantly increased inflammation and in particular, increased infiltration by macrophages. Consequently, depletion of macrophages in RAG1 KO or wild‐type mice led to decreased disease severity. On the contrary, depletion of Treg cells in wild‐type mice increased both psoriasis and the number of infiltrating macrophages, while adoptive transfer of Foxp3‐positive cells into RAG1 KO or wild‐type mice decreased both the development of psoriasis and macrophage infiltration. Thus, we conclude that Treg lymphocytes inhibit the pro‐inflammatory activity of macrophages, which are the major immune effector cells in hTNF ‐mediated psoriasis. Copyright © 2016 Pathological Society of Great Britain and Ireland. Published by John Wiley & Sons, Ltd.
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