The Il9 CNS-25 Regulatory Element Controls Mast Cell and Basophil IL-9 Production

IL-9 is an important mediator of allergic disease that is critical for mast cell-driven diseases. IL-9 is produced by many cell types, including T cells, basophils, and mast cells. Yet, how IL-9 is regulated in mast cells or basophils is not well characterized. In this report, we tested the effects of deficiency of a mouse gene regulatory element ( CNS-25) in these cells in vivo and in vitro. In mast cells stimulated with IL-3 and IL-33, the CNS-25 enhancer is a potent regulator of mast cell gene transcription and epigenetic modification at the locus. Our data show preferential binding of STAT5 and GATA1 to CNS-25 over the promoter in mast cells and that T cells and mast cells have differing requirements for the induction of IL-9 production. CNS-25 is required for IL-9 production from T cells, basophils, and mast cells in a food allergy model, and deficiency in IL-9 expression results in decreased mast cell expansion. In a infection model, we observed a similar decrease in mast cell accumulation. Although decreased mast cells correlated with higher parasite egg burden and delayed clearance in vivo, T cell deficiency in IL-9 also likely contributes to the phenotype. Thus, our data demonstrate IL-9 production in mast cells and basophils in vivo requires CNS-25, and that CNS-25-dependent IL-9 production is required for mast cell expansion during allergic intestinal inflammation.