Research ArticlePsoriasis

Gene from a Psoriasis Susceptibility Locus Primes the Skin for Inflammation

See allHide authors and affiliations

Science Translational Medicine  08 Dec 2010:
Vol. 2, Issue 61, pp. 61ra90
DOI: 10.1126/scitranslmed.3001108

You are currently viewing the abstract.

View Full Text

Log in to view the full text

Log in through your institution

Log in through your institution


Psoriasis is a common complex genetic disease characterized by hyperplasia and inflammation in the skin; however, the relative contributions of epidermal cells and the immune system to disease pathogenesis remain unclear. Linkage studies have defined a psoriasis susceptibility locus (PSORS4) on 1q21, the epidermal differentiation complex, which includes genes for small S100 calcium-binding proteins. These proteins are involved in extracellular and intracellular signaling during epithelial host defense, linking innate and adaptive immunity. Inflammation-prone psoriatic skin constitutively expresses elevated concentrations of S100A7 (psoriasin) and S100A15 (koebnerisin) in the epidermis. Here, we report that genetically modified mice expressing elevated amounts of doxycycline-regulated mS100a7a15 in skin keratinocytes demonstrated an exaggerated inflammatory response when challenged by exogenous stimuli such as abrasion (Koebner phenomenon). This immune response was characterized by immune cell infiltration and elevated concentrations of T helper 1 (TH1) and TH17 proinflammatory cytokines, which have been linked to the pathogenesis of psoriasis and were further amplified upon challenge. Both inflammation priming and amplification required mS100a7a15 binding to the receptor of advanced glycation end products (RAGE). mS100a7a15 potentiated inflammation by acting directly as a chemoattractant for leukocytes, further increasing the number of inflammatory cells infiltrating the skin. This study provides a pathogenetic psoriasis model using a psoriasis candidate gene to link the epidermis and innate immune system in inflammation priming, highlighting the S100A7A15-RAGE axis as a potential therapeutic target.


  • Citation: R. Wolf, F. Mascia, A. Dharamsi, O. M. Z. Howard, C. Cataisson, V. Bliskovski, J. Winston, L. Feigenbaum, U. Lichti, T. Ruzicka, T. Chavakis, S. H. Yuspa, Gene from a Psoriasis Susceptibility Locus Primes the Skin for Inflammation. Sci. Transl. Med. 2, 61ra90 (2010).

View Full Text

Stay Connected to Science Translational Medicine