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IL-9 as a mediator of Th17-driven inflammatory disease

机译:IL-9介导Th17驱动的炎症性疾病

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摘要

We report that like other T cells cultured in the presence of transforming growth factor (TGF) β, Th17 cells also produce interleukin (IL) 9. Th17 cells generated in vitro with IL-6 and TGF-β as well as purified ex vivo Th17 cells both produced IL-9. To determine if IL-9 has functional consequences in Th17-mediated inflammatory disease, we evaluated the role of IL-9 in the development and progression of experimental autoimmune encephalomyelitis, a mouse model of multiple sclerosis. The data show that IL-9 neutralization and IL-9 receptor deficiency attenuates disease, and this correlates with decreases in Th17 cells and IL-6–producing macrophages in the central nervous system, as well as mast cell numbers in the regional lymph nodes. Collectively, these data implicate IL-9 as a Th17-derived cytokine that can contribute to inflammatory disease.
机译:我们报告说,与在转化生长因子(TGF)β存在下培养的其他T细胞一样,Th17细胞也产生白介素(IL)9。用IL-6和TGF-β以及体外纯化的Th17体外生成的Th17细胞细胞均产生IL-9。为了确定IL-9在Th17介导的炎症性疾病中是否具有功能性后果,我们评估了IL-9在实验性自身免疫性脑脊髓炎(一种多发性硬化的小鼠模型)的发生和发展中的作用。数据显示,IL-9中和作用和IL-9受体缺乏会减弱疾病,这与中枢神经系统Th17细胞和产生IL-6的巨噬细胞减少以及区域淋巴结肥大细胞数量减少有关。总体而言,这些数据暗示IL-9是Th17衍生的细胞因子,可导致炎症性疾病。

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