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首页> 美国卫生研究院文献>Frontiers in Immunology >Synergy between Common γ Chain Family Cytokines and IL-18 Potentiates Innate and Adaptive Pathways of NK Cell Activation
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Synergy between Common γ Chain Family Cytokines and IL-18 Potentiates Innate and Adaptive Pathways of NK Cell Activation

机译:常见的γ链家族细胞因子和IL-18之间的协同作用增强了NK细胞活化的先天和适应性途径。

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Studies to develop cell-based therapies for cancer and other diseases have consistently shown that purified human natural killer (NK) cells secrete cytokines and kill target cells after in vitro culture with high concentrations of cytokines. However, these assays poorly reflect the conditions that are likely to prevail in vivo in the early stages of an infection and have been carried out in a wide variety of experimental systems, which has led to contradictions within the literature. We have conducted a detailed kinetic and dose–response analysis of human NK cell responses to low concentrations of IL-12, IL-15, IL-18, IL-21, and IFN-α, alone and in combination, and their potential to synergize with IL-2. We find that very low concentrations of both innate and adaptive common γ chain cytokines synergize with equally low concentrations of IL-18 to drive rapid and potent NK cell CD25 and IFN-γ expression; IL-18 and IL-2 reciprocally sustain CD25 and IL-18Rα expression in a positive feedback loop; and IL-18 synergizes with FcγRIII (CD16) signaling to augment antibody-dependent cellular cytotoxicity. These data indicate that NK cells can be rapidly activated by very low doses of innate cytokines and that the common γ chain cytokines have overlapping but distinct functions in combination with IL-18. Importantly, synergy between multiple signaling pathways leading to rapid NK cell activation at very low cytokine concentrations has been overlooked in prior studies focusing on single cytokines or simple combinations. Moreover, although the precise common γ chain cytokines available during primary and secondary infections may differ, their synergy with both IL-18 and antigen–antibody immune complexes underscores their contribution to NK cell activation during innate and adaptive responses. IL-18 signaling potentiates NK cell effector function during innate and adaptive immune responses by synergy with IL-2, IL-15, and IL-21 and immune complexes.
机译:开展针对癌症和其他疾病的基于细胞的疗法的研究一致表明,纯化的人类自然杀伤(NK)细胞在体外培养高浓度的细胞因子后会分泌细胞因子并杀死靶细胞。然而,这些测定法不能很好地反映出感染初期可能在体内普遍存在的状况,并且已经在各种各样的实验系统中进行了,这导致了文献中的矛盾。我们对人NK细胞对低浓度IL-12,IL-15,IL-18,IL-21和IFN-α的反应进行了详细的动力学和剂量反应分析,并分析了它们的潜力与IL-2协同作用。我们发现,非常低浓度的先天和适应性通用γ链细胞因子与同样低浓度的IL-18协同作用,以驱动快速有效的NK细胞CD25和IFN-γ表达。 IL-18和IL-2在正反馈回路中相互维持CD25和IL-18Rα表达。 IL-18与FcγRIII(CD16)信号传导协同作用,增强抗体依赖性细胞的细胞毒性。这些数据表明,NK细胞可以被极低剂量的先天细胞因子快速激活,并且常见的γ链细胞因子与IL-18结合具有重叠但截然不同的功能。重要的是,在专注于单一细胞因子或简单组合的先前研究中,导致极低细胞因子浓度的导致NK细胞快速活化的多种信号通路之间的协同作用已被忽略。此外,尽管在初次和继发感染期间可用的确切常见γ链细胞因子可能有所不同,但它们与IL-18和抗原-抗体免疫复合物的协同作用强调了它们在先天和适应性应答中对NK细胞活化的贡献。 IL-18信号传导通过与IL-2,IL-15和IL-21以及免疫复合物的协同作用,在先天性和适应性免疫应答过程中增强NK细胞效应子的功能。

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