IL‐33 is secreted by psoriatic keratinocytes and induces pro‐inflammatory cytokines via keratinocyte and mast cell activation |
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| Authors: | Anna Balato Serena Lembo Martina Mattii Maria Schiattarella Rita Marino Amato De Paulis Nicola Balato Fabio Ayala |
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| Affiliation: | 1. Department of Dermatology, University of Naples Federico II, , Naples, Italy;2. Department of Clinical Immunology and Allergy, University of Naples Federico II, , Naples, Italy;3. Technologies for Gene Expression Service, Stazione Zoologica Anton Dohrn, , Naples, Italy |
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| Abstract: | IL‐33 is a novel pro‐inflammatory cytokine and ligand for the orphan receptor ST2. Although originally defined as an inducer of Th2‐mediated responses, IL‐33 was recently found to be involved in arthritis, a Th1/Th17‐mediated disease. Here, we assessed the ability of IL‐33 to promote inflammation via mast cells (MCs) and keratinocytes (KCs) activation in psoriasis. IL‐33 resulted elevated in the skin but not in the serum of psoriasis patients. IL‐33 was secreted by psoriasis KCs and HaCaT cells after TNF‐α stimulation. In HMC‐1, TNF‐α, but not IL‐17, could induce a robust increase in IL‐33 expression. In HaCaT cells, TNF‐α was able to induce IL‐6, MCP‐1 and VEGF, and the addition of IL‐33 reinforced these increases. TNF‐α + IL‐33 combination showed similar results in primary KCs and ex vivo skin organ culture. In conclusion, our study suggests that IL‐33 may be involved in psoriasis biology via MCs and KCs. |
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| Keywords: | IL‐33 psoriasis |
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