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首页> 外文期刊>The journal of immunology >Fast Dendritic Cells Stimulated with Alternative Maturation Mixtures Induce Polyfunctional and Long-Lasting Activation of Innate and Adaptive Effector Cells with Tumor-Killing Capabilities
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Fast Dendritic Cells Stimulated with Alternative Maturation Mixtures Induce Polyfunctional and Long-Lasting Activation of Innate and Adaptive Effector Cells with Tumor-Killing Capabilities

机译:选择性成熟混合物刺激的快速树突状细胞诱导具有肿瘤杀伤能力的先天性和适应性效应细胞的多功能持久化激活

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摘要

The clinical usage of dendritic cells (DC) for tumor immunotherapy still requires improvements. In this study, three alternative maturation mixtures were compared with the cytokine-based gold standard, and the overall interaction of the resulting DC with effector cells from the innate as well as the adaptive immunity was evaluated in healthy donors. Stimulation with the TLR-4 ligand monophosphoryl lipid A together with IFN-γ (alt-2 DC) resulted in DC with the highest levels of costimulatory molecule expression and IL-12p70/IL-10 ratio. Whereas all alternative DC were able to induce NK and γδ T cells to acquire cytotoxic properties and secrete type 1 and proinflammatory cytokines, after both short (20-h)- and long (5–8 d)-time coculture, secretion of IFN-γ by the innate populations was induced in response to alt-2 and alt-1 DC (TNF-α, IFN-α, IFN-γ, IL-1β, poly IC), but not to alt-3 DC (TNF-α, IFN-γ, IL-1β, CL097). Regarding CD8+ T cell–mediated Ag-specific immune responses, a heterogeneous pattern of responses was obtained among the healthy donors, suggesting rather a competition than a synergy among the different effector cells. Our data promote further evaluation of alt-2 fast DC for translatability into clinical immunotherapy trials, while also fostering the need to identify biomarkers for immune cell responsiveness and tumor susceptibility to be able to select for each patient the best possible DC-based therapy.
机译:树突状细胞(DC)在肿瘤免疫治疗中的临床应用仍需要改进。在这项研究中,将三种替代的成熟混合物与基于细胞因子的金标准进行了比较,并在健康供体中评估了所得DC与先天效应细胞以及适应性免疫的总体相互作用。用TLR-4配体单磷酰脂质A和IFN-γ(alt-2 DC)刺激后,DC具有最高水平的共刺激分子表达和IL-12p70 / IL-10比。在短时间(20h)和长时间(5-8 d)共培养后,所有替代DC均可诱导NK和γδT细胞获得细胞毒性,并分泌1型和促炎性细胞因子,IFN-先天种群的γ是对alt-2和alt-1 DC(TNF-α,IFN-α,IFN-γ,IL-1β,poly IC)的应答,而不是对alt-3 DC(TNF-α)的诱导,IFN-γ,IL-1β,CL097)。关于CD8 + T细胞介导的Ag特异性免疫反应,在健康供体中获得了异质反应模式,这表明在不同效应细胞之间竞争而非协同作用。我们的数据促进了对alt-2快速DC在临床免疫治疗试验中的可翻译性的进一步评估,同时也促使人们需要确定免疫细胞反应性和肿瘤易感性的生物标志物,以便能够为每个患者选择最佳的基于DC的疗法。

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