Comparison of Vaccine-Induced Effector CD8 T Cell Responses Directed against Self- and Non-Self-Tumor Antigens: Implications for Cancer Immunotherapy

被引:55
|
作者
Pedersen, Sara R. [1 ]
Sorensen, Maria R. [1 ]
Buus, Soren [1 ]
Christensen, Jan P. [1 ]
Thomsen, Allan R. [1 ]
机构
[1] Univ Copenhagen, Dept Int Hlth Immunol & Microbiol, DK-2200 Copenhagen North, Denmark
来源
JOURNAL OF IMMUNOLOGY | 2013年 / 191卷 / 07期
关键词
INFILTRATING LYMPHOCYTES; MELANOMA; IMMUNITY; GP100; IMMUNIZATION; REGRESSION; TOLERANCE; THERAPY; EPITOPE; PD-1;
D O I
10.4049/jimmunol.1300555
中图分类号
R392 [医学免疫学]; Q939.91 [免疫学];
学科分类号
100102 ;
摘要
It is generally accepted that CD8 T cells play a major role in tumor control, yet vaccination aimed at eliciting potent CD8 T cell responses are rarely efficient in clinical trials. To try and understand why this is so, we have generated potent adenoviral vectors encoding the endogenous tumor Ags (TA) tyrosinase-related protein-2 (TRP-2) and glycoprotein 100 (GP100) tethered to the invariant chain (Ii). Using these vectors, we sought to characterize the self-TA-specific CD8 T cell response and compare it to that induced against non-self-Ags expressed from a similar vector platform. Prophylactic vaccination with adenoviral vectors expressing either TRP-2 (Ad-Ii-TRP-2) or GP100 (Ad-Ii-GP100) had little or no effect on the growth of s.c. B16 melanomas, and only Ad-Ii-TRP-2 was able to induce a marginal reduction of B16 lung metastasis. In contrast, vaccination with a similar vector construct expressing a foreign (viral) TA induced efficient tumor control. Analyzing the self-TA-specific CD8 T cells, we observed that these could be activated to produce IFN-gamma and TNF-alpha. In addition, surface expression of phenotypic markers and inhibitory receptors, as well as in vivo cytotoxicity and degranulation capacity matched that of non-self-Ag-specific CD8 T cells. However, the CD8 T cells specific for self-TAs had a lower functional avidity, and this impacted on their in vivo performance. On the basis of these results and a low expression of the targeted TA epitopes on the tumor cells, we suggest that low avidity of the self-TA-specific CD8 T cells may represent a major obstacle for efficient immunotherapy of cancer.
引用
收藏
页码:3955 / 3967
页数:13
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