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Interleukin(IL)-7Rα expression regulates murine dendritic cell sensitivity to Thymic Stromal Lymphopoietin

机译:白介素(IL)-7Rα表达调节小鼠树突状细胞对胸腺基质淋巴细胞生成素的敏感性

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摘要

Thymic stromal lymphopoietin (TSLP) and interleukin (IL)-7 are related cytokines that mediate growth and differentiation events in the immune system. They signal through IL-7Rα-containing receptors. Target cells of TSLP in Th2 responses include CD4 T cells and dendritic cells (DC's). While it has been reported that expression of TSLPR on CD4 T cells is required for OVA-induced lung inflammation, DC's have also been shown to be target cells of TSLP. We show here that murine ex vivo splenic DC's are unresponsive to TSLP, as they fail to phosphorylate STAT5, but in vitro overnight culture especially in presence of IL-4 renders DC's responsive to both TSLP and IL-7. This induced responsiveness is accompanied by dramatic upregulation of IL-7Rα on DC's with little change in expression of TSLPR or of γc. In splenic DC's, the induction of IL-7Rα occurs mainly in CD8 negative DC's. In vivo, we found that IL-4 has differential regulatory role on expression of IL-7Rα depending on the cell type; IL-4 decreases IL-7Rα expression on CD4 T cells while upregulating the expression on DC's. Our results indicate that the induction of IL-7Rα expression on DC's is critical for TSLP responsiveness and that IL-4 can upregulate IL-7Rα on DC's.
机译:胸腺基质淋巴细胞生成素(TSLP)和白介素(IL)-7是介导免疫系统中生长和分化事件的相关细胞因子。它们通过含有IL-7Rα的受体发出信号。 Th2反应中TSLP的靶细胞包括CD4 T细胞和树突状细胞(DC)。虽然已经报道了OVA诱导的肺部炎症需要在CD4 T细胞上表达TSLPR,但DC也已被证明是TSLP的靶细胞。我们在这里显示,鼠离体脾脏DC对TSLP无反应,因为它们无法磷酸化STAT5,但体外过夜培养尤其是在IL-4存在下使DC对TSLP和IL-7都有反应。这种诱导的反应性伴随着DC上IL-7Rα的急剧上调,而TSLPR或γc的表达变化很小。在脾脏DC中,IL-7Rα的诱导主要发生在CD8阴性DC中。在体内,我们发现IL-4对IL-7Rα的表达有不同的调节作用,具体取决于细胞类型。 IL-4降低CD4 T细胞上IL-7Rα的表达,同时上调DC上的表达。我们的结果表明,在DC上诱导IL-7Rα表达对于TSLP反应至关重要,并且IL-4可以在DC上调IL-7Rα。

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