首页> 外文期刊>Journal of Translational Medicine >Langerhans-type and monocyte-derived human dendritic cells have different susceptibilities to mRNA electroporation with distinct effects on maturation and activation: implications for immunogenicity in dendritic cell-based immunotherapy
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Langerhans-type and monocyte-derived human dendritic cells have different susceptibilities to mRNA electroporation with distinct effects on maturation and activation: implications for immunogenicity in dendritic cell-based immunotherapy

机译:Langerhans型和单核细胞衍生的人树突细胞对mRNA电穿孔具有不同的敏感性,其对成熟和活化的不同作用:在树突式细胞的免疫疗法中对免疫原性的影响

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Background mRNA electroporation of dendritic cells (DCs) facilitates processing and presentation of multiple peptides derived from whole antigen, tailored to different HLA molecules. Clinical responses to electroporated moDC vaccines, however, have been suboptimal. Human Langerhans-type DCs (LCs) are the most potent conventional DC subtype for inducing CD8+ cytotoxic T lymphocytes (CTLs) in vitro. We recently demonstrated that Wilms’ tumor 1 (WT1) mRNA-electroporated LCs are superior to moDCs as stimulators of tumor antigen-specific CD8+ CTLs, even though they are comparable stimulators of allogeneic T cell proliferative responses. A detailed comparative evaluation of the effects of mRNA electroporation on LCs versus moDCs, however, is needed. Methods Immature and partially-matured human moDCs and LCs electroporated with mRNA were compared for transfection efficiency, phenotypic changes, viability, retention of transgene expression after cryopreservation, and immunogenicity. Student t test was used for each pairwise comparison. One-way analysis of variance was used for multiple group comparisons. Results Transfection efficiency after electroporation with enhanced green fluorescent protein (eGFP) mRNA was higher for immature than for partially-matured moDCs. In contrast, transfection efficiency was higher for partially-matured than for immature LCs, with the additional benefit that electroporation itself increased maturation and activation of CD83+HLA-DRbright LCs but not moDCs. Electroporation did not impair final maturation and activation of either DC subtype, after which both mRNA-electroporated LCs and moDCs were functionally similar in stimulating allogeneic T cell proliferation, a standard assay of DC immunogenicity. Conclusions These findings support mRNA electroporation of DCs, and in particular LCs, as an effective non-viral method to stimulate specific, potent CD8+ CTL responses. The differences between LCs and moDCs regarding this form of antigen-loading have important implications for DC-based immunotherapies.
机译:树突细胞(DCS)的背景MRNA电穿孔促进了来自整个抗原的多种肽的加工和呈递,针对不同的HLA分子定制。然而,对电穿孔的ModC疫苗的临床反应已经次优。人朗格汉斯型DCS(LCS)是最有效的常规DC亚型,用于在体外诱导CD8 + 细胞毒性T淋巴细胞(CTL)。我们最近证明,Wilms肿瘤1(WT1)mRNA电穿孔LCS优于MODC,作为肿瘤抗原特异性CD8 + CTL的刺激剂,即使它们是同种异体T细胞增殖反应的类似刺激器。然而,需要对MRNA电穿孔对LCS与MODC的影响进行详细的比较评价。方法对MORNA电穿孔的未成熟和部分成熟的人MODCS和LCS进行比较,以转染效率,表型变化,活力,在冷冻保存后的转基因表达的保留,以及免疫原性。学生T测试用于每对成对比较。单向分析方差分析用于多组比较。结果与部分成熟的ModCs具有增强的绿色荧光蛋白(EGFP)mRNA电穿孔后的转染效率。相反,部分成熟的转染效率高于未成熟的LCS,电穿孔本身增加了CD83 + HLA-DR BRIGHT LCS但是的额外益处不是modcs。电穿孔不损害DC亚型的最终成熟和活化,之后MRNA电穿孔LC和MODC在刺激同种异体T细胞增殖中的功能性相似,DC免疫原性的标准测定。结论这些发现支持DCS的MRNA电穿孔,特别是LCS,作为刺激特异性,有效的CD8 + / SOP> CTL响应的有效非病毒方法。 LCS和MODCS关于这种形式的抗原负载的差异对基于DC的免疫疗法具有重要意义。

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