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Interleukin-4 therapy of psoriasis induces Th2 responses and improves human autoimmune disease
Authors:Ghoreschi Kamran  Thomas Peter  Breit Susanne  Dugas Martin  Mailhammer Reinhard  van Eden Willem  van der Zee Ruurd  Biedermann Tilo  Prinz Jörg  Mack Matthias  Mrowietz Ulrich  Christophers Enno  Schlöndorff Detlef  Plewig Gerd  Sander Christian A  Röcken Martin
Affiliation:Department of Dermatology and Allergology, Ludwig-Maximilians University Munich, Munich, Germany.
Abstract:Selective skewing of autoreactive interferon-gamma (IFN-gamma)-producing T helper cells (Th1) toward an interleukin-4 (IL-4)-producing (Th2) phenotype can in experimental animals alleviate autoimmune disease without inducing general immunosuppression. In a prospective dose escalation study, we assessed treatment with human IL-4 (rhuIL-4) in 20 patients with severe psoriasis. The therapy was well tolerated, and within six weeks all patients showed decreased clinical scores and 15 improved more than 68%. Stable reduction of clinical scores was significantly better at 0.2-0.5 microg rhuIL-4 than at < or =0.1 microg rhuIL-4 (P = 0.009). In psoriatic lesions, treatment with 0.2-0.5 microg/kg rhuIL-4 reduced the concentrations of IL-8 and IL-19, two cytokines directly involved in psoriasis; the number of chemokine receptor CCR5+ Th1 cells; and the IFN-gamma/IL-4 ratio. In the circulation, 0.2-0.5 microg/kg rhuIL-4 increased the number of IL-4+CD4+ T cells two- to three-fold. Thus, IL-4 therapy can induce Th2 differentiation in human CD4+ T cells and has promise as a potential treatment for psoriasis, a prototypic Th1-associated autoimmune disease.
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