4.7 Article

Interleukin-29 induces epithelial production of CXCR3A ligands and T-cell infiltration

Journal

JOURNAL OF MOLECULAR MEDICINE-JMM
Volume 94, Issue 4, Pages 391-400

Publisher

SPRINGER HEIDELBERG
DOI: 10.1007/s00109-015-1367-y

Keywords

Cytokine; Chemokine; Skin disease; Infiltration; Interferon-lambda; Biomarker

Funding

  1. German Research Foundation (Deutsche Forschungsgemeinschaft) [WO 1567/1-1/2, SA1868/2]
  2. Federal Ministry of Education and Research (Bundesministerium fur Bildung und Forschung) [01ZX1312A]

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Psoriasis is considered as a model for chronic immune-mediated disorders. Th17-cells are pivotal players in those diseases. Recently, we demonstrated that Th17-cells produce interleukin (IL)-29 and that IL-29 is highly present in psoriatic lesions. Whether IL-29, with its action on epithelial cells and melanocytes, contributes to psoriasis pathogenesis, was unknown so far. Analysis of IL-29-treated human keratinocytes revealed induction of the chemokines CXCL10, CXCL11, and, to a much lesser extent, CXCL9. Unlike these CXCR3A ligands, known to attract Th1-, CD8(+), NK-, and Th1/Th17 transient cells, no influence was found on chemokines attracting other immune cell populations or on molecules modulating the CXCR3A/CXCR3A ligand interaction. CXCR3A ligand expression was also induced by IL-29 in melanocytes and in epidermis models and explanted skin. Regarding other psoriasis-relevant cytokines, interferon-gamma and, less potently, tumor necrosis factor-alpha and IL-1 beta shared and strengthened IL-29's capacity. Murine IL-29 counterpart injected into mouse skin provoked local CXCL10 and CXCL11 expression, T-cell infiltration, and, in consequence, skin swelling. The elevated IL-29 expression in psoriatic lesions was associated with upregulation of CXCR3A ligands compared to non-lesional skin of these patients and to the skin of healthy donors and atopic dermatitis patients, which lack IL-29 production. Importantly, neutralization of IL-29 reduced CXCR3A ligand levels in explant cultures of psoriatic lesions. Finally, elevated blood CXCL11 levels were found in psoriasis that might be useful for monitoring lesional activity of the IL-29 axis. In summary, the Th17-cytokine IL-29 induces specific chemokines and, in consequence, provokes skin infiltration of potentially pathogenic T-cells.

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