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High dose CD11c-driven IL15 is sufficient to drive NK cell maturation and anti-tumor activity in a trans-presentation independent manner

机译:高剂量CD11c驱动的IL15足以以独立于转位方式的方式驱动NK细胞成熟和抗肿瘤活性

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摘要

The common gamma (γc)-chain cytokine interleukin 15 (IL15) is a multifunctional immune-modulator which impacts the generation, maturation and activity of many cell types of the innate, as well as the adaptive immune system, including natural killer (NK) and CD8+ T cells. Using a new series of transgenic mice, we analyzed the in vivo potential of IL15 as an immune-regulator when available at different concentrations or delivery modes, i.e. soluble monomer or complexed to its specific receptor α (Rα)-chain. We have identified distinct effects on selected IL15-responsive populations. While CD8+ T cells required complexed forms of IL15/IL15Rα for full functionality, mature NK populations were rescued in an IL15/IL15Rα-deficient environment by high levels of CD11c-restricted IL15. These IL15-conditions were sufficient to limit tumor formation in a lung metastasis model indicating that the NK cell populations were fully functional. These data underline the potential of “free” IL15 in the absence of Rα-complex as a powerful and specific immuno-modulator, which may be beneficial where selective immune-activation is desired.
机译:常见的γ(γc)链细胞因子白介素15(IL15)是一种多功能的免疫调节剂,可影响先天性多种细胞类型的生成,成熟和活性以及包括自然杀手(NK)在内的适应性免疫系统和CD8 + T细胞。使用一系列新的转基因小鼠,我们分析了IL15在不同浓度或递送方式(即可溶性单体或与其特异性受体α(Rα)链复合)可用时作为免疫调节剂的体内潜力。我们已经发现对选定的IL15反应人群的独特影响。 CD8 + T细胞需要复杂形式的IL15 /IL15Rα才能发挥全部功能,而成熟的NK群体则通过高水平的CD11c限制性IL15在IL15 /IL15Rα缺乏的环境中得以拯救。这些IL15条件足以限制肺转移模型中的肿瘤形成,表明NK细胞群体具有充分的功能。这些数据强调了在不存在Rα-复合物的情况下“游离” IL15作为强大而特异性的免疫调节剂的潜力,这在需要选择性免疫激活的地方可能是有益的。

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