首页> 外文期刊>Journal of immunotherapy >IL-12 secreting dendritic cells are required for optimum activation of human secondary lymphoid tissue T cells.
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IL-12 secreting dendritic cells are required for optimum activation of human secondary lymphoid tissue T cells.

机译:分泌IL-12的树突状细胞是人类次级淋巴组织T细胞最佳活化所必需的。

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摘要

Successful immunization requires that mature dendritic cells (mDCs) prime T cells in secondary lymphoid tissue (LT). Previously, the authors have shown that LT T cell activation has an increased costimulatory threshold for a proliferative response as compared with peripheral blood (PB) T cells. Therefore, to optimize mDC immunogenicity, DC maturation was studied using LT T cells as responders. While mDCs obtained with soluble CD40Ligand (sCD40L) or a sCD40L/IFNgamma combination similarly expressed the CD83 and CCR7 molecules on their membrane, only the latter secreted IL-12. sCD40L/IFNgamma mDCs, as compared with sCD40L mDCs, enhanced allogeneic LT T cell proliferation, LT CD4+ cell IFNgamma production and LT CD8+ cell cytotoxicity. Enhancement could be predominantly ascribed to IL-12 secreted by sCD40L/IFNgamma mDCs and to additional costimulatory signals as shown remarkably in the IFNgamma response when IL-12 was neutralized. Therefore, in addition to their membrane phenotype, mDCs to be used in immunization protocols should be assessed for IL-12 secretion as a surrogate marker for an optimum costimulatory potential.
机译:成功的免疫要求成熟的树突状细胞(mDC)引发次级淋巴组织(LT)中的T细胞。先前,作者已经表明,与外周血(PB)T细胞相比,LT T细胞的激活具有增殖反应的共刺激阈值。因此,为了优化mDC的免疫原性,使用LT T细胞作为应答剂研究了DC成熟。用可溶性CD40Ligand(sCD40L)或sCD40L / IFNgamma组合获得的mDC类似地在其膜上表达CD83和CCR7分子,但只有后者分泌IL-12。与sCD40L mDC相比,sCD40L /IFNγmDC增强了同种异体LT T细胞增殖,LT CD4 +细胞IFNγ的产生和LT CD8 +细胞的细胞毒性。增强可能主要归因于sCD40L / IFNgamma mDC分泌的IL-12以及附加的共刺激信号,如中和IL-12时的IFNgamma响应所示。因此,除了其膜表型外,还应评估免疫方案中使用的mDC的IL-12分泌,以作为最佳共刺激潜力的替代标志。

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