Laboratoire d'Immunologie, Institut Curie, Paris, France.
J Immunol. 2010 Jul 15;185(2):892-901. doi: 10.4049/jimmunol.1000933. Epub 2010 Jun 11.
The optimization of anticancer therapeutic vaccines can lead to better efficacy but also to stronger adverse effects. In a mouse model of antitumor vaccination using a long peptide (LP), which included MHC class I- and II-restricted male (H-Y) epitopes, we observed unexpected mortality. Mice with an increased frequency of anti-H-Y CD4 T cells were primed with LP+CpG and boosted 10 d later. Within hours of boost, they displayed shock-like signs with high mortality. Serum cytokine levels were high. TNF-alpha secreted by the CD4 T cells was identified as the key effector molecule. Priming with a short peptide (SP), which included the MHC class II-restricted epitope, was a more efficient primer than LP, but did not lead to mortality when used as boost. The high mortality induced by LP compared with SP was probably related to its specific ability to be presented by B cells. Finally, targeting the LP sequence to dendritic cells allowed tumor protection without side effects. Our data: 1) confirm that the immune system can be very dangerous; 2) caution against the use of systemic activation of high-frequency Ag-specific T cells as induced by high doses of LP; and 3) underline the benefit of targeting Ag to dendritic cells.
抗癌治疗性疫苗的优化可以提高疗效,但也会导致更强的不良反应。在使用长肽(LP)进行抗肿瘤疫苗接种的小鼠模型中,我们观察到了意外的死亡率。具有较高频率抗-H-Y CD4 T 细胞的小鼠用 LP+CpG 进行了初始免疫,并在 10 天后进行了加强免疫。在加强免疫后数小时内,它们出现了类似休克的症状,死亡率很高。血清细胞因子水平升高。CD4 T 细胞分泌的 TNF-α被鉴定为关键效应分子。用包括 MHC 类 II 限制性表位的短肽(SP)进行初始免疫比 LP 更有效,但作为加强免疫时不会导致死亡。与 SP 相比,LP 引起的高死亡率可能与其被 B 细胞呈递的特定能力有关。最后,将 LP 序列靶向树突状细胞可在没有副作用的情况下保护肿瘤。我们的数据:1)证实免疫系统可能非常危险;2)警告不要使用高剂量 LP 诱导的全身性激活高频率 Ag 特异性 T 细胞;3)强调将 Ag 靶向树突状细胞的益处。
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