从冷冻保存的癌症患者PBMC中产生的成熟MDDC的表型和体外功能与来自健康供体的MDDC相当。

Journal of immune based therapies and vaccines Pub Date : 2007-05-03 DOI:10.1186/1476-8518-5-7

Smita A Ghanekar, Sonny Bhatia, Joyce J Ruitenberg, Corazon DeLa Rosa, Mary L Disis, Vernon C Maino, Holden T Maecker, Cory A Waters

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引用次数: 19

摘要

背景:单核细胞衍生的树突状细胞(MDDC)是基于疫苗的多种癌症临床研究中使用的主要DC类型。为了评估从冷冻保存的癌症患者PBMC中体外分化的MDDC是否在功能上与健康供者不同，我们比较了这些细胞的共刺激和功能标记的表达。此外，还利用健康供体的样本评估了PBMC前体冷冻保存对MDDC质量的影响。方法:使用流式细胞术，我们比较了正常供体和癌症患者在GM-CSF+IL-4(未成熟MDDC)和GM-CSF+IL-4+TNFalpha+ il -1 β +IL-6+PGE-2(成熟MDDC)存在下生长的MDDC (a)表面表型如CD209、CD83和CD86， (b)细胞内功能标记如IL-12和环氧化酶-2 (COX-2)， (c)分泌IL-8和IL-12的能力，以及(d)刺激异体和抗原特异性自体T细胞的能力。结果:前体冷冻保存确实影响MDDC标志物的表达，但只有CD86和COX-2两种标志物受到显著影响。来自健康供体和癌症患者的成熟MDDC上调CD83、CD86的表达、IL-12+和COX-2+细胞的频率以及IL-8的分泌;并且相对于未成熟细胞下调CD209的表达。与健康供体相比，来自癌症患者的成熟MDDC在几乎所有研究标记物的表达上都是相同的，重要的是，它们在体外刺激同种异体和抗原特异性T细胞的能力是相同的。结论:我们的数据显示，DC前体的低温保存对大多数MDDC标记物没有显著影响，尽管有减少共刺激制造者和细胞因子表达的趋势。此外，来自癌症患者冷冻保存的PBMC的单核细胞可以完全分化为成熟的DC，其表型和功能与来自健康供体的DC相同。

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Phenotype and in vitro function of mature MDDC generated from cryopreserved PBMC of cancer patients are equivalent to those from healthy donors.

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Phenotype and in vitro function of mature MDDC generated from cryopreserved PBMC of cancer patients are equivalent to those from healthy donors.

Background: Monocyte-derived-dendritic-cells (MDDC) are the major DC type used in vaccine-based clinical studies for a variety of cancers. In order to assess whether in vitro differentiated MDDC from cryopreserved PBMC of cancer patients are functionally distinct from those of healthy donors, we compared these cells for their expression of co-stimulatory and functional markers. In addition, the effect of cryopreservation of PBMC precursors on the quality of MDDC was also evaluated using samples from healthy donors.

Methods: Using flow cytometry, we compared normal donors and cancer patients MDDC grown in the presence of GM-CSF+IL-4 (immature MDDC), and GM-CSF+IL-4+TNFalpha+IL-1beta+IL-6+PGE-2 (mature MDDC) for (a) surface phenotype such as CD209, CD83 and CD86, (b) intracellular functional markers such as IL-12 and cyclooxygenase-2 (COX-2), (c) ability to secrete IL-8 and IL-12, and (d) ability to stimulate allogeneic and antigen-specific autologous T cells.

Results: Cryopreservation of precursors did affect MDDC marker expression, however, only two markers, CD86 and COX-2, were significantly affected. Mature MDDC from healthy donors and cancer patients up-regulated the expression of CD83, CD86, frequencies of IL-12+ and COX-2+ cells, and secretion of IL-8; and down-regulated CD209 expression relative to their immature counterparts. Compared to healthy donors, mature MDDC generated from cancer patients were equivalent in the expression of nearly all the markers studied and importantly, were equivalent in their ability to stimulate allogeneic and antigen-specific T cells in vitro.

Conclusion: Our data show that cryopreservation of DC precursors does not significantly affect the majority of the MDDC markers, although the trends are towards reduced expression of co-stimulatory makers and cytokines. In addition, monocytes from cryopreserved PBMC of cancer patients can be fully differentiated into mature DC with phenotype and function equivalent to those derived from healthy donors.

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Journal of immune based therapies and vaccines

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