Institute of Infection and Immunity, Cardiff University School of Medicine , Cardiff , UK.
NIHR Biomedical Research Unit, Centre for Liver Research, University of Birmingham Medical School , Birmingham , UK.
Front Immunol. 2014 Jul 23;5:344. doi: 10.3389/fimmu.2014.00344. eCollection 2014.
Cell-based immunotherapy strategies target tumors directly (via cytolytic effector cells) or aim at mobilizing endogenous anti-tumor immunity. The latter approach includes dendritic cells (DC) most frequently in the form of in vitro cultured peripheral blood monocytes-derived DC. Human blood γδT cells are selective for a single class of non-peptide agonists ("phosphoantigens") and develop into potent antigen-presenting cells (APC), termed γδT-APC within 1-3 days of in vitro culture. Availability of large numbers of γδT-APC would be advantageous for use as a novel cellular vaccine. We here report optimal γδT cell expansion (>10(7) cells/ml blood) when peripheral blood mononuclear cells (PBMC) from healthy individuals and melanoma patients were stimulated with zoledronate and then cultured for 14 days in the presence of IL-2 and IL-15, yielding γδT cell cultures of variable purity (77 ± 21 and 56 ± 26%, respectively). They resembled effector memory αβT (TEM) cells and retained full functionality as assessed by in vitro tumor cell killing as well as secretion of pro-inflammatory cytokines (IFNγ, TNFα) and cell proliferation in response to stimulation with phosphoantigens. Importantly, day 14 γδT cells expressed numerous APC-related cell surface markers and, in agreement, displayed potent in vitro APC functions. Day 14 γδT cells from PBMC of patients with cancer were equally effective as their counterparts derived from blood of healthy individuals and triggered potent CD8(+) αβT cell responses following processing and cross-presentation of simple (influenza M1) and complex (tuberculin purified protein derivative) protein antigens. Of note, and in clear contrast to peripheral blood γδT cells, the ability of day 14 γδT cells to trigger antigen-specific αβT cell responses did not depend on re-stimulation. We conclude that day 14 γδT cell cultures provide a convenient source of autologous APC for use in immunotherapy of patients with various cancers.
基于细胞的免疫治疗策略直接针对肿瘤(通过细胞毒性效应细胞)或旨在动员内源性抗肿瘤免疫。后一种方法包括树突状细胞(DC),最常以体外培养的外周血单核细胞衍生的 DC 的形式存在。人类血液 γδT 细胞对一类非肽激动剂(“磷酸抗原”)具有选择性,并在体外培养 1-3 天内发展成为有效的抗原呈递细胞(APC),称为 γδT-APC。大量 γδT-APC 的可用性将有利于用作新型细胞疫苗。我们在此报告了当健康个体和黑色素瘤患者的外周血单核细胞(PBMC)用唑来膦酸刺激,然后在 IL-2 和 IL-15 的存在下培养 14 天时,γδT 细胞的最佳扩增(>10(7)细胞/ml 血液),产生的 γδT 细胞培养物纯度不同(分别为 77±21%和 56±26%)。它们类似于效应记忆 αβT(TEM)细胞,并通过体外肿瘤细胞杀伤以及分泌促炎细胞因子(IFNγ、TNFα)和对磷酸抗原刺激的细胞增殖来保持完全功能。重要的是,第 14 天的 γδT 细胞表达了许多 APC 相关的细胞表面标志物,并且与体外 APC 功能强大一致。来自癌症患者 PBMC 的第 14 天 γδT 细胞与来自健康个体血液的对应细胞同样有效,并在处理和交叉呈递简单(流感 M1)和复杂(结核菌素纯蛋白衍生物)蛋白抗原后触发强烈的 CD8(+)αβT 细胞反应。值得注意的是,与外周血 γδT 细胞形成鲜明对比的是,第 14 天 γδT 细胞触发抗原特异性 αβT 细胞反应的能力不依赖于再刺激。我们得出结论,第 14 天的 γδT 细胞培养物为各种癌症患者的免疫治疗提供了方便的自体 APC 来源。
Zotero 插件
