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Evidence that a neutrophil–keratinocyte crosstalk is an early target of IL‐17A inhibition in psoriasis
Authors:Kristian Reich  Kim A. Papp  Robert T. Matheson  John H. Tu  Robert Bissonnette  Marc Bourcier  David Gratton  Rodion A. Kunynetz  Yves Poulin  Les A. Rosoph  Georg Stingl  Wolfgang M. Bauer  Janeen M. Salter  Thomas M. Falk  Norbert A. Blödorn‐Schlicht  Wolfgang Hueber  Ulrike Sommer  Thomas Peters  Ernst Kriehuber  David M. Lee  Grazyna A. Wieczorek  Frank Kolbinger  Conrad C. Bleul
Affiliation:1. Dermatologikum Hamburg and SCIderm Research Institute, Hamburg, Germany;2. Probity Medical Research Inc, Waterloo, ON, Canada;3. Oregon Medical Research Center PC, Portland, OR, USA;4. Skin Search of Rochester, Rochester, NY, USA;5. Innovaderm Research Inc, Montreal, QC, Canada;6. Dermatology Clinic, Moncton, NB, Canada;7. International Dermatology Research, Montreal, QC, Canada;8. Ultranova Skincare, Barrie, ON, Canada;9. Centre de Recherche Dermatologique du Québec Métropolitain, Quebec City, QC, Canada;10. North Bay Dermatology Centre, North Bay, ON, Canada;11. Division of Immunology, Allergy and Infectious Diseases, Department of Dermatology, Medical University of Vienna, Vienna, Austria;12. Novartis Institutes for BioMedical Research, Basel, Switzerland
Abstract:The response of psoriasis to antibodies targeting the interleukin (IL)‐23/IL‐17A pathway suggests a prominent role of T‐helper type‐17 (Th17) cells in this disease. We examined the clinical and immunological response patterns of 100 subjects with moderate‐to‐severe psoriasis receiving 3 different intravenous dosing regimens of the anti‐IL‐17A antibody secukinumab (1 × 3 mg/kg or 1 × 10 mg/kg on Day 1, or 3 × 10 mg/kg on Days 1, 15 and 29) or placebo in a phase 2 trial. Baseline biopsies revealed typical features of active psoriasis, including epidermal accumulation of neutrophils and formation of microabscesses in >60% of cases. Neutrophils were the numerically largest fraction of infiltrating cells containing IL‐17 and may store the cytokine preformed, as IL‐17A mRNA was not detectable in neutrophils isolated from active plaques. Significant clinical responses to secukinumab were observed 2 weeks after a single infusion, associated with extensive clearance of cutaneous neutrophils parallel to the normalization of keratinocyte abnormalities and reduction of IL‐17‐inducible neutrophil chemoattractants (e.g. CXCL1, CXCL8); effects on numbers of T cells and CD11c‐positive dendritic cells were more delayed. Histological and immunological improvements were generally dose dependent and not observed in the placebo group. In the lowest‐dose group, a recurrence of neutrophils was seen in some subjects at Week 12; these subjects relapsed faster than those without microabscesses. Our findings are indicative of a neutrophil–keratinocyte axis in psoriasis that may involve neutrophil‐derived IL‐17 and is an early target of IL‐17A‐directed therapies such as secukinumab.
Keywords:IL‐17A  neutrophils  psoriasis  secukinumab
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