4.5 Review

T cell pathology in skin inflammation

Journal

SEMINARS IN IMMUNOPATHOLOGY
Volume 41, Issue 3, Pages 359-377

Publisher

SPRINGER HEIDELBERG
DOI: 10.1007/s00281-019-00742-7

Keywords

Skin inflammation; Immune-mediated disease; IL-4; IL-17; IL-22; IFN-; TNF-; TGF-

Funding

  1. Deutsche Forschungsgemeinschaft (DFG) [FOR 2497/TP02, GH133/2-1]
  2. German Federal Ministry of Education and Research [01ZX1312A]
  3. Novartis Pharma GmbH

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Forming the outer body barrier, our skin is permanently exposed to pathogens and environmental hazards. Therefore, skin diseases are among the most common disorders. In many of them, the immune system plays a crucial pathogenetic role. For didactic and therapeutic reasons, classification of such immune-mediated skin diseases according to the underlying dominant immune mechanism rather than to their clinical manifestation appears to be reasonable. Immune-mediated skin diseases may be mediated mainly by T cells, by the humoral immune system, or by uncontrolled unspecific inflammation. According to the involved T cell subpopulation, T cell-mediated diseases may be further subdivided into T1 cell-dominated (e.g., vitiligo), T2 cell-dominated (e.g., acute atopic dermatitis), T17/T22 cell-dominated (e.g., psoriasis), and Treg cell-dominated (e.g., melanoma) responses. Moreover, T cell-dependent and -independent responses may occur simultaneously in selected diseases (e.g., hidradenitis suppurativa). The effector mechanisms of the respective T cell subpopulations determine the molecular changes in the local tissue cells, leading to specific microscopic and macroscopic skin alterations. In this article, we show how the increasing knowledge of the T cell biology has been comprehensively translated into the pathogenetic understanding of respective model skin diseases and, based thereon, has revolutionized their daily clinical management.

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