Protective low-avidity anti-tumour CD8+ T cells are selectively attenuated by regulatory T cells.

IF 4.1 Q2 IMMUNOLOGY Immunotherapy advances Pub Date : 2020-11-25 eCollection Date: 2021-01-01 DOI:10.1093/immadv/ltaa001
Gessa Sugiyarto, David Prossor, Osman Dadas, E David Arcia-Anaya, Tim Elliott, Edward James
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引用次数: 3

Abstract

Objectives: Regulatory T cells (Treg) play a major role in the suppression of protective anti-tumour T cell responses. In the CT26 BALB/c murine model of colorectal carcinoma, Tregs differentially suppress responses to two characterised CD8+ T epitopes, AH1 and GSW11, which results in an absence of detectable IFN-γ-producing GSW11-specific T cells in the spleen and lymph nodes of tumour challenged mice. Activation of GSW11-specific T cells correlates with protection against tumour progression. We wanted to examine the presence of non-functional GSW11-specific T cells in Treg replete and depleted mice, assess their phenotype and their affinity compared to AH1-specific T cells.

Methods: We used peptide-specific tetramers to identify tumour-specific CD8+ T cells and assessed the cell surface expression of markers associated with exhaustion (PD-1, Tim3 and Lag-3) and their function by IFN-g production using flow cytometry. We also assessed the T cell receptor (TcR) clonality of tumour-specific T cells. Tetramer competition assays were performed to determine the relative affinity of identified TcR.

Results: Here, we show that GSW11-specific T cells are in fact induced in Treg-replete, CT26-bearing mice, where they make up the majority of tumour-infiltrating CD8+ lymphocytes, but exhibit an 'exhausted' phenotype. This dysfunctional phenotype is induced early in the anti-tumour response in tumours. Depletion of Tregs prior to tumour challenge correlates with an altered T cell receptor (TcR) repertoire. Moreover, the avidity of GSW11-specific TcRs that expanded in the absence of Tregs was significantly lower compared with TcRs of CD8+populations that were diminished in protective anti-tumour responses.

Conclusion: Our results indicate that Tregs suppress the induction of protective anti-tumour T cell responses and may signify that low-avidity T cells play an important role in this protection.

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保护性低亲和性抗肿瘤CD8+ T细胞被调节性T细胞选择性地减弱。
目的:调节性T细胞(Treg)在抑制保护性抗肿瘤T细胞反应中发挥重要作用。在CT26 BALB/c小鼠结直肠癌模型中,Tregs不同程度地抑制了对两种CD8+ T表位AH1和GSW11的反应,导致肿瘤小鼠脾脏和淋巴结中检测不到产生IFN-γ的GSW11特异性T细胞。激活gsw11特异性T细胞与防止肿瘤进展相关。我们想要检查Treg充满和耗尽小鼠中非功能性gsw11特异性T细胞的存在,评估它们的表型及其与ah1特异性T细胞的亲和力。方法:我们使用肽特异性四聚体鉴定肿瘤特异性CD8+ T细胞,并使用流式细胞术评估与衰竭相关的标志物(PD-1, Tim3和Lag-3)的细胞表面表达及其通过IFN-g产生的功能。我们还评估了肿瘤特异性T细胞的T细胞受体(TcR)克隆性。采用四聚体竞争法测定鉴定的TcR的相对亲和力。结果:在这里,我们发现gsw11特异性T细胞实际上在treg -充满ct26的小鼠中被诱导,其中它们构成了大多数肿瘤浸润的CD8+淋巴细胞,但表现出“耗尽”表型。这种功能失调的表型在肿瘤抗肿瘤反应的早期被诱导。肿瘤攻击前Tregs的消耗与T细胞受体(TcR)库的改变有关。此外,与在保护性抗肿瘤反应中减少的CD8+群体的tcr相比,在缺乏Tregs的情况下扩增的gsw11特异性tcr的贪婪度显着降低。结论:我们的研究结果表明Tregs抑制了保护性抗肿瘤T细胞反应的诱导,可能表明低亲和力T细胞在这种保护中起重要作用。
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