首页> 美国卫生研究院文献>Springer Open Choice >Controlled-rate freezer cryopreservation of highly concentrated peripheral blood mononuclear cells results in higher cell yields and superior autologous T-cell stimulation for dendritic cell-based immunotherapy
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Controlled-rate freezer cryopreservation of highly concentrated peripheral blood mononuclear cells results in higher cell yields and superior autologous T-cell stimulation for dendritic cell-based immunotherapy

机译:高浓度外周血单个核细胞的控制速率冰箱冷冻保存可提高细胞产量并为基于树突细胞的免疫疗法带来卓越的自体T细胞刺激

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摘要

Availability of large quantities of functionally effective dendritic cells (DC) represents one of the major challenges for immunotherapeutic trials against infectious or malignant diseases. Low numbers or insufficient T-cell activation of DC may result in premature termination of treatment and unsatisfying immune responses in clinical trials. Based on the notion that cryopreservation of monocytes is superior to cryopreservation of immature or mature DC in terms of resulting DC quantity and immuno-stimulatory capacity, we aimed to establish an optimized protocol for the cryopreservation of highly concentrated peripheral blood mononuclear cells (PBMC) for DC-based immunotherapy. Cryopreserved cell preparations were analyzed regarding quantitative recovery, viability, phenotype, and functional properties. In contrast to standard isopropyl alcohol (IPA) freezing, PBMC cryopreservation in an automated controlled-rate freezer (CRF) with subsequent thawing and differentiation resulted in significantly higher cell yields of immature and mature DC. Immature DC yields and total protein content after using CRF were comparable with results obtained with freshly prepared PBMC and exceeded results of standard IPA freezing by approximately 50 %. While differentiation markers, allogeneic T-cell stimulation, viability, and cytokine profiles were similar to DC from standard freezing procedures, DC generated from CRF-cryopreserved PBMC induced a significantly higher antigen-specific IFN-γ release from autologous effector T cells. In summary, automated controlled-rate freezing of highly concentrated PBMC represents an improved method for increasing DC yields and autologous T-cell stimulation.
机译:大量功能有效的树突状细胞(DC)的可用性代表了针对传染性或恶性疾病的免疫治疗试验的主要挑战之一。 DC的数量少或T细胞活化不足可能会导致治疗过早终止,并且临床试验中的免疫反应无法令人满意。基于单核细胞冷冻保存优于未成熟或成熟DC冷冻保存的DC量和免疫刺激能力的观点,我们旨在建立一种用于冷冻保存高浓度外周血单核细胞(PBMC)的优化方案。基于DC的免疫疗法。分析冷冻保存的细胞制品的定量回收率,生存力,表型和功能特性。与标准异丙醇(IPA)冷冻不同,PBMC在自动控制速率冷冻机(CRF)中冷冻保存并随后解冻和分化可显着提高未成熟DC和成熟DC的细胞产量。使用CRF后未成熟的DC产量和总蛋白含量与新鲜制备的PBMC所获得的结果相当,并且比标准IPA冷冻的结果超出了约50%。尽管分化标记,同种异体T细胞刺激,生存力和细胞因子谱与标准冷冻程序的DC相似,但CRF低温保存的PBMC产生的DC诱导自体效应T细胞释放的抗原特异性IFN-γ明显更高。总之,高浓度PBMC的自动控制速率冷冻代表了一种提高DC产量和自体T细胞刺激的改进方法。

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