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CTLA-4 blockade during dendritic cell based booster vaccination influences dendritic cell survival and CTL expansion

机译:基于树突细胞的加强免疫接种期间的CTLA-4阻断影响树突细胞存活和CTL扩增

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Dendritic cells (DCs) are potent antigen-presenting cells and critical for the priming of CD8+ T cells. Therefore the use of these cells as adjuvant cells has been tested in a large number of experimental and clinical vaccination studies, in particular cancer vaccine studies. A number of protocols are emerging that combine vaccination with CTL expanding strategies, such as e.g. blockade of CTLA-4 signalling. On the other hand, the lifespan and in vivo survival of therapeutic DCs have only been addressed in a few studies, although this is of importance for the kinetics of CTL induction during vaccination. We have previously reported that DCs loaded with specific antigens are eliminated by antigen specific CTLs in vivo and that this elimination affects the potential for in vivo CTL generation. We now show that CTLA-4 blockade increases the number of DC vaccine induced LCMV gp33 specific CTLs and the lysis of relevant in vivo targets. However, the CTLA-4 blockage dependent expansion of CTLs also affect DC survival during booster DC injections and our data suggest that during a booster DC vaccine, the largest increase in CTL levels is already obtained during the first vaccination.
机译:树突状细胞(DC)是有效的抗原呈递细胞,对于启动CD8 + T细胞至关重要。因此,已经在大量的实验和临床疫苗接种研究中,特别是在癌症疫苗研究中,测试了将这些细胞用作佐剂细胞。出现了将疫苗接种与CTL扩展策略相结合的多种协议,例如封锁CTLA-4信号。另一方面,治疗性DC的寿命和体内存活仅在少数研究中得到解决,尽管这对于疫苗接种过程中CTL诱导的动力学很重要。我们以前曾报道过,负载有特定抗原的DC在体内被抗原特异性CTL消除,并且这种消除影响了体内CTL产生的可能性。现在,我们显示CTLA-4封锁增加了DC疫苗诱导的LCMV gp33特异性CTL的数量以及相关体内靶标的裂解。但是,CTLA-4阻断依赖性CTL的扩增也会影响DC加强注射期间的DC存活,我们的数据表明,在DC加强疫苗期间,首次接种期间CTL的增加最大。

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