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Publication : A Novel Role for IL-6 Receptor Classic Signaling: Induction of ROR<i>γ</i>t<sup>+</sup>Foxp3<sup>+</sup> Tregs with Enhanced Suppressive Capacity.

First Author  Hagenstein J Year  2019
Journal  J Am Soc Nephrol Volume  30
Issue  8 Pages  1439-1453
PubMed ID  31311828 Mgi Jnum  J:294466
Mgi Id  MGI:6456509 Doi  10.1681/ASN.2019020118
Citation  Hagenstein J, et al. (2019) A Novel Role for IL-6 Receptor Classic Signaling: Induction of RORgammat(+)Foxp3(+) Tregs with Enhanced Suppressive Capacity. J Am Soc Nephrol 30(8):1439-1453
abstractText  BACKGROUND: New therapies blocking the IL-6 receptor (IL-6R) have recently become available and are successfully being used to treat inflammatory diseases like arthritis. Whether IL-6 blockers may help patients with kidney inflammation currently remains unknown. METHODS: To learn more about the complex role of CD4(+) T cell-intrinsic IL-6R signaling, we induced nephrotoxic nephritis, a mouse model for crescentic GN, in mice lacking T cell-specific IL-6Ra. We used adoptive transfer experiments and studies in reporter mice to analyze immune responses and Treg subpopulations. RESULTS: Lack of IL-6Ra signaling in mouse CD4(+) T cells impaired the generation of proinflammatory Th17 cells, but surprisingly did not ameliorate the course of GN. In contrast, renal damage was significantly reduced by restricting IL-6Ra deficiency to T effector cells and excluding Tregs. Detailed studies of Tregs revealed unaltered IL-10 production despite IL-6Ra deficiency. However, in vivo and in vitro, IL-6Ra classic signaling induced RORgammat(+)Foxp3(+) double-positive Tregs (biTregs), which carry the trafficking receptor CCR6 and have potent immunoregulatory properties. Indeed, lack of IL-6Ra significantly reduced Treg in vitro suppressive capacity. Finally, adoptive transfer of T cells containing IL-6Ra(-/-) Tregs resulted in severe aggravation of GN in mice. CONCLUSIONS: Our data refine the old paradigm, that IL-6 enhances Th17 responses and suppresses Tregs. We here provide evidence that T cell-intrinsic IL-6Ra classic signaling indeed induces the generation of Th17 cells but at the same time highly immunosuppressive RORgammat(+) biTregs. These results advocate caution and indicate that IL-6-directed therapies for GN need to be cell-type specific.
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