IL-17A Production by Renal γδ T Cells Promotes Kidney Injury in Crescentic GN
2012; American Society of Nephrology; Volume: 23; Issue: 9 Linguagem: Inglês
10.1681/asn.2012010040
ISSN1533-3450
AutoresJan‐Eric Turner, Christian F. Krebs, André P. Tittel, Hans‐Joachim Paust, Catherine Meyer-Schwesinger, Sabrina B. Bennstein, Oliver M. Steinmetz, Immo Prinz, Tim Magnus, Thomas Korn, Rolf A.K. Stahl, Christian Kurts, Ulf Panzer,
Tópico(s)Dermatology and Skin Diseases
ResumoThe Th17 immune response appears to contribute to the pathogenesis of human and experimental crescentic GN, but the cell types that produce IL-17A in the kidney, the mechanisms involved in its induction, and the IL-17A-mediated effector functions that promote renal tissue injury are incompletely understood. Here, using a murine model of crescentic GN, we found that CD4(+) T cells, γδ T cells, and a population of CD3(+)CD4(-)CD8(-)γδT cell receptor(-)NK1.1(-) T cells all produce IL-17A in the kidney. A time course analysis identified γδ T cells as a major source of IL-17A in the early phase of disease, before the first CD4(+) Th17 cells arrived. The production of IL-17A by renal γδ T cells depended on IL-23p19 signaling and retinoic acid-related orphan receptor-γt but not on IL-1β or IL-6. In addition, depletion of dendritic cells, which produce IL-23 in the kidney, reduced IL-17A production by renal γδ T cells. Furthermore, the lack of IL-17A production in γδ T cells, as well as the absence of all γδ T cells, reduced neutrophil recruitment into the kidney and ameliorated renal injury. Taken together, these data suggest that γδ T cells produce IL-17A in the kidney, induced by IL-23, promoting neutrophil recruitment, and contributing to the immunopathogenesis of crescentic GN.
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