分泌XCL1的癌胚抗原嵌合抗原受体T细胞增强内源性CD8 T细胞对肿瘤新抗原的反应,以赋予长期抗肿瘤免疫力。
XCL1-secreting CEA CAR-T cells enhance endogenous CD8 T cell responses to tumor neoantigens to confer a long-term antitumor immunity.
作者信息
Li Xing-Ning, Wang Feifei, Chen Kun, Wu Zhiyuan, Zhang Ruochan, Xiao Chentong, Zhao Fei, Wang Dongmei, Zhao Hong, Ran Yuliang, Qu Chunfeng
机构信息
Immunology Department, National Cancer Center/National Clinical Research Center for Cancer/Cancer Hospital, Chinese Academy of Medical Sciences and Peking Union Medical College, Beijing, China.
Immunology Department, State Key Lab of Molecular Oncology, National Cancer Center/National Clinical Research Center for Cancer/Cancer Hospital, Chinese Academy of Medical Sciences and Peking Union Medical College, Beijing, China
出版信息
J Immunother Cancer. 2025 Jan 6;13(1):e010581. doi: 10.1136/jitc-2024-010581.
BACKGROUND
Therapeutic efficacy of carcinoembryonic antigen (CEA)-specific chimeric antigen receptor (CAR) T cells against colorectal cancer (CRC) remains limited due to the unique characteristics and distinct microenvironments of tumor tissues. We modified CEA-specific CAR-T cells, aiming to stimulate endogenous CD8 T cell responses against neoantigens that were derived from CEA-positive tumors destroyed by the CAR T cells.
METHODS
In a conventional CEA CAR (reg-CAR), we modified it to express lymphotactin XCL1 and interleukin (IL)-7 genes, constructing a modified 7XCL1-CAR. By generating the CEA-specific 7XCL1-CAR T cells, we assessed their antitumor efficacy against CRC cells with varying levels of CEA expression, both in cell-cultures and in two strains of tumor-bearing syngeneic mice.
RESULTS
Following retroviral transduction, 7XCL1-CAR T cells and reg-CAR T cells exhibited similar positive proportions of CEA-CAR and CD4:CD8 ratios. In co-culture system with CEA-negative CT26 cells, no differences in cytotoxicity were observed between 7XCL1-CAR and reg-CAR T cells. However, in co-culture with CT26.CEA and CT26.CEA cells, 7XCL1-CAR T cells displayed higher cytotoxicity than that reg-CAR T cells after 60 hours. On interaction with CT26.CEA-positive cells, 7XCL1-CAR T cells secreted higher levels of XCL1 and IL-7, effectively recruited the most potent cross-presenting cDC1s (type-I conventional dendritic cells), and sustained the antitumor activity of CAR-T cells. In treating mice that carried tumors derived from universally CEA-positive cells, 7XCL1-CAR T cells exhibited no difference compared with reg-CAR T cells. However, in treating mice with tumors containing both CEA-positive and CEA-negative cells, 7XCL1-CAR T cells displayed greater inhibition than that of reg-CAR-T cells. After treatment of 7XCL1-CAR T cells, tumor-bearing mice exhibited enhanced infiltration of cDC1s, maintained CAR-T activity, and generation of endogenous neoantigen-specific T cells. Consequently, 7XCL1-CAR T cell-treated mice demonstrated resistance to challenge with CEA-negative CT26 cells.
CONCLUSION
Treatment with CEA-specific, XCL1-secreting CAR-T cells for CEA-positive tumors promoted the generation of CD8 T cells against tumor neoantigens, mediating a long-term antitumor immunity against heterogeneous CRCs.
背景
由于肿瘤组织的独特特征和不同微环境,癌胚抗原(CEA)特异性嵌合抗原受体(CAR)T细胞对结直肠癌(CRC)的治疗效果仍然有限。我们对CEA特异性CAR-T细胞进行了改造,旨在刺激内源性CD8 T细胞对由CAR T细胞破坏的CEA阳性肿瘤衍生的新抗原产生反应。
方法
在传统的CEA CAR(reg-CAR)中,我们对其进行改造以表达淋巴细胞趋化因子XCL1和白细胞介素(IL)-7基因,构建了一种改造后的7XCL1-CAR。通过生成CEA特异性的7XCL1-CAR T细胞,我们在细胞培养和两种荷瘤同基因小鼠品系中评估了它们对不同CEA表达水平的CRC细胞的抗肿瘤疗效。
结果
经逆转录病毒转导后,7XCL1-CAR T细胞和reg-CAR T细胞在CEA-CAR阳性比例和CD4:CD8比值方面表现相似。在与CEA阴性的CT26细胞共培养系统中,7XCL1-CAR和reg-CAR T细胞在细胞毒性方面未观察到差异。然而,在与CT26.CEA和CT26.CEA细胞共培养时,60小时后7XCL1-CAR T细胞显示出比reg-CAR T细胞更高的细胞毒性。与CT26.CEA阳性细胞相互作用时,7XCL1-CAR T细胞分泌更高水平的XCL1和IL-7,有效招募最有效的交叉呈递cDC1s(I型传统树突状细胞),并维持CAR-T细胞的抗肿瘤活性。在治疗源自普遍CEA阳性细胞的肿瘤的小鼠时,7XCL1-CAR T细胞与reg-CAR T细胞相比没有差异。然而,在治疗含有CEA阳性和CEA阴性细胞的肿瘤的小鼠时,7XCL1-CAR T细胞显示出比reg-CAR-T细胞更大的抑制作用。用7XCL1-CAR T细胞治疗后,荷瘤小鼠表现出cDCs1浸润增强、CAR-T活性维持以及内源性新抗原特异性T细胞的产生。因此,经7XCL1-CAR T细胞治疗的小鼠对CEA阴性的CT26细胞攻击具有抗性。
结论
用分泌XCL1的CEA特异性CAR-T细胞治疗CEA阳性肿瘤可促进针对肿瘤新抗原的CD8 T细胞的产生,介导对异质性CRC的长期抗肿瘤免疫。
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