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The biological basis of disease recurrence in psoriasis: a historical perspective and current models

L. Puig, Antonio Costanzo, Ernesto J. Muñoz‐Elías, Maria Jazra, Sven Wegner, C. Paul, Curdin Conrad

2021British Journal of Dermatology105 citationsDOIOpen Access PDF

Abstract

tissue-resident memory T cells in resolved skin, which can initiate and perpetuate immune responses of psoriasis in the absence of T-cell recruitment from the blood. Dendritic cells (DCs) are antigen-presenting cells that contribute to psoriasis pathology via the secretion of IL-23, the upstream regulator of Th17 cells, while plasmacytoid DCs are involved via IL-36 signalling and type I interferon activation. Overall, the evidence discussed in this review indicates that IL-23-driven/IL-17-producing T cells play a critical role in psoriasis pathology and recurrence, making these cytokines logical therapeutic targets. The review also explains the clinical efficacy of IL-17 and IL-23 receptor blockers in the treatment of psoriasis.

Topics & Concepts

PsoriasisImmunologyMedicinePlasmacytoid dendritic cellCD8DiseaseImmune systemPopulationInterleukin 17InflammationDendritic cellPathologyEnvironmental healthPsoriasis: Treatment and PathogenesisDermatology and Skin DiseasesT-cell and B-cell Immunology
The biological basis of disease recurrence in psoriasis: a historical perspective and current models | Litcius