TCF1 阳性和 TCF1 阴性 TRM CD8 T 细胞亚群和 cDC1 协调黑色素瘤保护和免疫治疗反应。
TCF1-positive and TCF1-negative TRM CD8 T cell subsets and cDC1s orchestrate melanoma protection and immunotherapy response.
机构信息
Posgrado en Ciencias Biológicas, Facultad de Medicina, Universidad Nacional Autónoma de México, Mexico City, Mexico.
Unidad de Investigación Médica en Inmunoquímica, UMAE Hospital de Especialidades, Centro Médico Nacional Siglo XXI, Instituto Mexicano del Seguro Social, Ciudad de Mexico, Mexico.
出版信息
J Immunother Cancer. 2024 Jul 5;12(7):e008739. doi: 10.1136/jitc-2023-008739.
BACKGROUND
Melanoma, the most lethal form of skin cancer, has undergone a transformative treatment shift with the advent of checkpoint blockade immunotherapy (CBI). Understanding the intricate network of immune cells infiltrating the tumor and orchestrating the control of melanoma cells and the response to CBI is currently of utmost importance. There is evidence underscoring the significance of tissue-resident memory (TRM) CD8 T cells and classic dendritic cell type 1 (cDC1) in cancer protection. Transcriptomic studies also support the existence of a + (encoding TCF1) T cell as the most important for immunotherapy response, although uncertainty exists about whether there is a TCF1+TRM T cell due to evidence indicating TCF1 downregulation for tissue residency activation.
METHODS
We used multiplexed immunofluorescence and spectral flow cytometry to evaluate TRM CD8 T cells and cDC1 in two melanoma patient cohorts: one immunotherapy-naive and the other receiving immunotherapy. The first cohort was divided between patients free of disease or with metastasis 2 years postdiagnosis while the second between CBI responders and non-responders.
RESULTS
Our study identifies two CD8+TRM subsets, TCF1+ and TCF1-, correlating with melanoma protection. TCF1+TRM cells show heightened expression of IFN-γ and Ki67 while TCF1- TRM cells exhibit increased expression of cytotoxic molecules. In metastatic patients, TRM subsets undergo a shift in marker expression, with the TCF1- subset displaying increased expression of exhaustion markers. We observed a close spatial correlation between cDC1s and TRMs, with TCF1+TRM/cDC1 pairs enriched in the stroma and TCF1- TRM/cDC1 pairs in tumor areas. Notably, these TCF1- TRMs express cytotoxic molecules and are associated with apoptotic melanoma cells. Both TCF1+ and TCF1- TRM subsets, alongside cDC1, prove relevant to CBI response.
CONCLUSIONS
Our study supports the importance of TRM CD8 T cells and cDC1 in melanoma protection while also highlighting the existence of functionally distinctive TCF1+ and TCF1- TRM subsets, both crucial for melanoma control and CBI response.
背景
黑色素瘤是最致命的皮肤癌形式,随着检查点阻断免疫疗法(CBI)的出现,它经历了治疗方式的重大转变。了解浸润肿瘤的免疫细胞的复杂网络,并协调对黑色素瘤细胞的控制以及对 CBI 的反应,目前至关重要。有证据表明组织驻留记忆(TRM)CD8 T 细胞和经典树突状细胞 1(cDC1)在癌症保护中具有重要作用。转录组学研究还支持 +(编码 TCF1)T 细胞的存在对于免疫治疗反应最重要,尽管由于存在 TCF1 下调以激活组织驻留的证据,对于是否存在 TCF1+TRM T 细胞存在不确定性。
方法
我们使用多重免疫荧光和光谱流式细胞术评估了两个黑色素瘤患者队列中的 TRM CD8 T 细胞和 cDC1:一个是免疫治疗初治的,另一个是接受免疫治疗的。第一个队列根据患者在诊断后 2 年是否无疾病或转移分为两组,第二个队列根据 CBI 反应者和非反应者分为两组。
结果
我们的研究确定了两个 CD8+TRM 亚群,TCF1+和 TCF1-,与黑色素瘤的保护有关。TCF1+TRM 细胞表现出 IFN-γ 和 Ki67 的高表达,而 TCF1-TRM 细胞表现出细胞毒性分子的高表达。在转移性患者中,TRM 亚群的标志物表达发生变化,TCF1-亚群的衰竭标志物表达增加。我们观察到 cDC1 和 TRM 之间存在密切的空间相关性,TCF1+TRM/cDC1 对在基质中富集,而 TCF1-TRM/cDC1 对在肿瘤区域富集。值得注意的是,这些 TCF1-TRM 表达细胞毒性分子,与凋亡的黑色素瘤细胞相关。TCF1+和 TCF1-TRM 亚群以及 cDC1 均与 CBI 反应相关。
结论
我们的研究支持 TRM CD8 T 细胞和 cDC1 在黑色素瘤保护中的重要性,同时也强调了功能不同的 TCF1+和 TCF1-TRM 亚群的存在,这两者对于黑色素瘤的控制和 CBI 反应都至关重要。
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