A non-functional neoepitope specific CD8+ T-cell response induced by tumor derived antigen exposure in vivo

被引:14
|
作者
Vormehr, Mathias [1 ,2 ]
Reinhard, Katharina [1 ]
Blatnik, Renata [3 ,4 ]
Josef, Kathrin [3 ,4 ]
Beck, Jan David [5 ]
Salomon, Nadja [5 ]
Suchan, Martin [5 ]
Selmi, Abderraouf [5 ]
Vascotto, Fulvia [5 ]
Zerweck, Johannes [6 ]
Wenschuh, Holger [6 ]
Diken, Mustafa [1 ,5 ]
Kreiter, Sebastian [1 ,5 ]
Tureci, Ozlem [1 ]
Riemer, Angelika B. [3 ,4 ]
Sahin, Ugur [1 ,2 ,5 ]
机构
[1] Biopharmaceut New Technol BioNTech Corp, Mainz, Germany
[2] Johannes Gutenberg Univ Mainz, Expt & Translat Oncol, Univ Med Ctr, Mainz, Germany
[3] German Canc Res Ctr, Immunotherapy & Immunoprevent, Heidelberg, Germany
[4] German Ctr Infect Res DZIF, Mol Vaccine Design, Heidelberg, Germany
[5] Johannes Gutenberg Univ gGmbH, TRON Translat Oncol, Univ Med Ctr, Mainz, Germany
[6] JPT Peptide Technol GmbH, Berlin, Germany
来源
ONCOIMMUNOLOGY | 2019年 / 8卷 / 03期
关键词
Neoepitopes; CD8(+) T cells; cancer immunotherapy; T cell priming; CD8(+) T cell cytotoxicity; CROSS-PRESENTATION; CTLA-4; BLOCKADE; PD-1; NEO-ANTIGENS; RECEPTOR; IMMUNOTHERAPY; RECOGNITION; SENSITIVITY; IPILIMUMAB; STABILITY;
D O I
10.1080/2162402X.2018.1553478
中图分类号
R73 [肿瘤学];
学科分类号
100214 ;
摘要
Cancer-associated mutations, mostly single nucleotide variations, can act as neoepitopes and prime targets for effective anti-cancer T-cell immunity. T cells recognizing cancer mutations are critical for the clinical activity of immune checkpoint blockade (ICB) and they are potent vaccine antigens. High frequencies of mutation-specific T cells are rarely spontaneously induced. Hence, therapies that broaden the tumor specific T-cell response are of interest. Here, we analyzed neoepitope-specific CD8(+) T-cell responses mounted either spontaneously or after immunotherapy regimens, which induce local tumor inflammation and cell death, in mice bearing tumors of the widely used colon carcinoma cell line CT26. A comprehensive immune reactivity screening of 2474 peptides covering 628 transcribed CT26 point mutations was conducted. All tested treatment regimens were found to induce a single significant CD8(+) T-cell response against a non-synonymous D733A point mutation in the Smc3 gene. Surprisingly, even though Smc3 D733A turned out to be the immune-dominant neoepitope in CT26 tumor bearing mice, neither T cells specific for this neoepitope nor their T cell receptors (TCRs) were able to recognize or lyse tumor cells. Moreover, vaccination with the D733A neoepitope did not result in anti-tumoral activity despite induction of specific T cells. This is to our knowledge the first report that neoepitope specific CD8(+) T cells primed by tumor-released antigen exposure in vivo can be functionally irrelevant.
引用
收藏
页数:14
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