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Invariant chain as a vehicle to load antigenic peptides on human MHC class I for cytotoxic T-cell activation

机译:不变的链作为车辆负载抗原人力MHC类我肽细胞毒性t细胞激活

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摘要

Protective T-cell responses depend on efficient presentation of antigen (Ag) in the context of major histocompatibility complex class I (MHCI) and class II (MHCII) molecules. Invariant chain (Ii) serves as a chaperone for MHCII molecules and mediates trafficking to the endosomal pathway. The genetic exchange of the class II-associated Ii peptide (CLIP) with antigenic peptides has proven efficient for loading of MHCII and activation of specific CD4+ T cells. Here, we investigated if Ii could similarly activate human CD8+ T cells when used as a vehicle for cytotoxic T-cell (CTL) epitopes. The results show that wild type Ii, and Ii in which CLIP was replaced by known CTL epitopes from the cancer targets MART-1 or CD20, coprecipitated with HLA-A*02:01 and mediated colocalization in the endosomal pathway. Furthermore, HLA-A*02:01-positive cells expressing CLIP-replaced Ii efficiently activated Ag-specific CD8+ T cells in a TAP- and proteasome-independent manner. Finally, dendritic cells transfected with mRNA encoding IiMART-1 or IiCD20 primed na?ve CD8+ T cells. The results show that Ii carrying antigenic peptides in the CLIP region can promote efficient presentation of the epitopes to CTLs independently of the classical MHCI peptide loading machinery, facilitating novel vaccination strategies against cancer.
机译:保护t细胞反应取决于效率表示抗原(Ag)的上下文中主要组织相容性复合体一级(MHCI)和二级(MHCII)分子。(2)作为MHCII分子伴侣endosomal和介导贩卖途径。II-associated Ii抗原肽(夹)肽已被证明有效的加载MHCII和激活特定的CD4 + T细胞。在这里,我们如果Ii可以类似的调查激活当用作人类CD8 + T细胞细胞毒性t细胞(CTL)抗原表位的工具。结果表明,野生型二世和Ii剪辑是取代了CTL的抗原表位癌症目标MART-1或CD20,共沉淀与抗原* 02:01 colocalization在介导的endosomal通路。于* 02:01-positive细胞表达CLIP-replaced Ii有效激活Ag-specific丝锥,CD8 + T细胞proteasome-independent方式。细胞转染与信使rna编码IiMART-1或IiCD20影射na吗?显示二世携带的抗原肽剪辑区域能促进有效的演讲独立ctl表位的古典MHCI肽装载机械、促进新型疫苗接种策略癌症。

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