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Th1 cytokines are more effective than Th2 cytokines at licensing anti-tumour functions in CD40-activated human macrophages in vitro

机译:比Th2 Th1细胞因子更有效细胞因子在许可抗肿瘤功能CD40-activated人类巨噬细胞体外

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摘要

CD40 agonists are showing activity in early clinical trials in patients with advanced cancer. In animal models, CD40 agonists synergise with T-cell-activating therapies to inhibit tumour growth by driving tumour macrophage repolarisation from an immunosuppressive to a Th1 immunostimulatory, tumouricidal phenotype. We therefore tested the hypothesis that T-cell-derived cytokines license anti-tumour functions in CD40-activated human macrophages. CD40 ligand (CD40L) alone activated macrophages to produce immunosuppressive IL-10, in a similar fashion to bacterial LPS, but failed to promote anti-tumour functions. The Th1 cytokine IFN-γ optimally licensed CD40L-induced macrophage anti-tumour functions, inducing a switch from IL-10 to IL-12p70 production, promoting macrophage-mediated Th1 T-cell skewing and enhancing tumouricidal activity. We found that even the Th2 cytokines IL-4 and IL-13 promoted IL-12p70 production (albeit without inhibiting IL-10 production) and enhanced Th1 T-cell skewing by CD40L-activated macrophages. However, IL-4 and IL-13 did not enhance tumouricidal activity in CD40L-activated macrophages. Thus, while both Th1 and Th2 cytokines biased macrophages to a Th1 immunostimulatory phenotype, only Th1 cytokines promoted tumouricidal activity in CD40L-activated macrophages. The presence of tumour-infiltrating Th1 or Th2 cells might therefore be predictive for patient response to CD40 agonism.
机译:在早期CD40受体激动剂显示出活动对晚期癌症患者的临床试验。在动物模型中,CD40受体激动剂把T-cell-activating疗法抑制肿瘤增长推动肿瘤巨噬细胞Th1 repolarisation的免疫抑制免疫刺激性,tumouricidal表型。因此测试的假设T-cell-derived抗肿瘤细胞因子许可证CD40-activated人类巨噬细胞功能。CD40配体(CD40L)单独激活巨噬细胞产生免疫抑制il - 10,在一个类似的时尚细菌有限合伙人,但未能推广抗肿瘤的功能。最优许可CD40L-induced巨噬细胞抗肿瘤功能,诱导一个开关il - 10 IL-12p70生产,推广macrophage-mediated Th1 t细胞扭曲加强tumouricidal活动。甚至连Th2细胞因子il - 4和IL-13晋升IL-12p70生产(尽管没有抑制il - 10生产)和增强Th1 t细胞扭曲CD40L-activated巨噬细胞。IL-13没有增强tumouricidal活动CD40L-activated巨噬细胞。和Th2 Th1细胞因子有偏见的巨噬细胞免疫刺激性表型,只有Th1细胞因子促进了CD40L-activated tumouricidal活动巨噬细胞。Th1、Th2细胞可能因此预测患者应对CD40激动。

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