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Publication : Regulatory T cells enhance mast cell production of IL-6 via surface-bound TGF-β.

First Author  Ganeshan K Year  2012
Journal  J Immunol Volume  188
Issue  2 Pages  594-603
PubMed ID  22156492 Mgi Jnum  J:180880
Mgi Id  MGI:5308128 Doi  10.4049/jimmunol.1102389
Citation  Ganeshan K, et al. (2012) Regulatory T cells enhance mast cell production of IL-6 via surface-bound TGF-beta. J Immunol 188(2):594-603
abstractText  Mast cell degranulation is a hallmark of allergic reactions, but mast cells can also produce many cytokines that modulate immunity. Recently, CD25(+) regulatory T cells (Tregs) have been shown to inhibit mast cell degranulation and anaphylaxis, but their influence on cytokine production remained unknown. In this study, we show that, rather than inhibit, Tregs actually enhance mast cell production of IL-6. We demonstrate that, whereas inhibition of degranulation was OX40/OX40 ligand dependent, enhancement of IL-6 was due to TGF-beta. Interestingly, our data demonstrate that the Treg-derived TGF-beta was surface-bound, because the interaction was contact dependent, and no TGF-beta was detectable in the supernatant. Soluble TGF-beta1 alone was sufficient to enhance mast cell IL-6 production, and these supernatants were sufficient to promote Th17 skewing, but those from Treg-mast cell cultures were not, supporting this being surface-bound TGF-beta from the Tregs. Interestingly, the augmentation of IL-6 production occurred basally or in response to innate stimuli (LPS or peptidoglycan), adaptive stimuli (IgE cross-linking by specific Ag), and cytokine activation (IL-33). We demonstrate that TGF-beta led to enhanced transcription and de novo synthesis of IL-6 upon activation without affecting IL-6 storage or mRNA stability. In vivo, the adoptive transfer of Tregs inhibited mast cell-dependent anaphylaxis in a model of food allergy but promoted intestinal IL-6 and IL-17 production. Consequently, our findings establish that Tregs can exert divergent influences upon mast cells, inhibiting degranulation via OX40/OX40 ligand interactions while promoting IL-6 via TGF-beta.
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