NK Receptor Signaling Lowers TCR Activation Threshold, Enhancing Selective Recognition of Cancer Cells by TAA-Specific CTLs.

IF 8.1 1区 医学 Q1 IMMUNOLOGY
Bowen Dong, Nataša Obermajer, Takemasa Tsuji, Junko Matsuzaki, Cindy M Bonura, Cindy Sander, Henry Withers, Mark D Long, Colin Chavel, Scott H Olejniczak, Hans Minderman, John M Kirkwood, Robert P Edwards, Walter J Storkus, Pedro Romero, Pawel Kalinski
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Abstract

Cytotoxic CD8+ T lymphocyte (CTL) recognition of non-mutated tumor-associated antigens (TAA), present on cancer cells and also in healthy tissues, is an important element of cancer immunity, but the mechanism of its selectivity for cancer cells and opportunities for its enhancement remain elusive. In this study, we found that CTL expression of the NK receptors (NKR) DNAM1 and NKG2D was associated with the effector status of CD8+ tumor-infiltrating lymphocytes and long-term survival of patients with melanoma. Using MART1 and NY-ESO-1 as model TAAs, we demonstrated that DNAM1 and NKG2D regulate T-cell receptor (TCR) functional avidity and set the threshold for TCR activation of human TAA-specific CTLs. Superior co-stimulatory effects of DNAM1 over CD28 involved enhanced TCR signaling, CTL killer function, and polyfunctionality. Double transduction of human CTLs with TAA-specific TCR and NKRs resulted in strongly enhanced antigen sensitivity, without a reduction in antigen specificity and selectivity of killer function. In addition, the elevation of NKR ligand expression on cancer cells due to chemotherapy also increased CTL recognition of cancer cells expressing low levels of TAAs. Our data help explain the ability of self-antigens to mediate tumor rejection in the absence of autoimmunity and support the development of dual-targeting adoptive T-cell therapies that use NKRs to enhance the potency and selectivity of recognition of TAA-expressing cancer cells.

NK 受体信号降低 TCR 激活阈值,增强 TAA 特异性 CTL 对癌细胞的选择性识别。
CTL识别存在于癌细胞上但也存在于健康组织中的非变异肿瘤相关抗原(TAA)是癌症免疫的一个重要因素,但其对癌细胞的选择性机制及其增强机会仍未确定。在这项研究中,我们发现NK受体(NKR)DNAM-1和NKG2D的CTL表达与CD8+肿瘤浸润淋巴细胞(TIL)的效应状态和黑色素瘤患者的长期生存有关。以MART-1和NY-ESO-1为模型TAA,我们证明了DNAM-1和NKG2D能调节T细胞受体(TCR)的功能热敏性,并设定了TCR激活人类TAA特异性CTL的阈值。DNAM-1比CD28更优越的成本刺激效应包括增强TCR信号、CTL杀伤功能和多功能性。用 TAA 特异性 TCR 和 NKRs 双重转导人类 CTL 可显著提高抗原敏感性,而不会降低抗原特异性和杀伤功能的选择性。此外,化疗提高了癌细胞上 NKR 配体的表达,也增加了 CTL 对表达低水平 TAA 的癌细胞的识别能力。我们的数据有助于解释自身抗原在没有自身免疫的情况下介导肿瘤排斥反应的能力,并支持利用 NKRs 提高识别表达 TAA 的癌细胞的效力和选择性的双靶点领养 T 细胞疗法的开发。
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来源期刊
Cancer immunology research
Cancer immunology research ONCOLOGY-IMMUNOLOGY
CiteScore
15.60
自引率
1.00%
发文量
260
期刊介绍: Cancer Immunology Research publishes exceptional original articles showcasing significant breakthroughs across the spectrum of cancer immunology. From fundamental inquiries into host-tumor interactions to developmental therapeutics, early translational studies, and comprehensive analyses of late-stage clinical trials, the journal provides a comprehensive view of the discipline. In addition to original research, the journal features reviews and opinion pieces of broad significance, fostering cross-disciplinary collaboration within the cancer research community. Serving as a premier resource for immunology knowledge in cancer research, the journal drives deeper insights into the host-tumor relationship, potent cancer treatments, and enhanced clinical outcomes. Key areas of interest include endogenous antitumor immunity, tumor-promoting inflammation, cancer antigens, vaccines, antibodies, cellular therapy, cytokines, immune regulation, immune suppression, immunomodulatory effects of cancer treatment, emerging technologies, and insightful clinical investigations with immunological implications.
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