抗原非依赖激活对于 GUCY2C 靶向 CAR-T 细胞的持久抗肿瘤效果至关重要。
Antigen-independent activation is critical for the durable antitumor effect of GUCY2C-targeted CAR-T cells.
机构信息
State Key Laboratory of Holistic Integrative Management of Gastrointestinal Cancers, Beijing Key Laboratory of Carcinogenesis and Translational Research, Department of Early Drug Development Centre, Peking University Cancer Hospital, Beijing, China
Beijing Imunopharm Technology Co Ltd, Beijing, China.
出版信息
J Immunother Cancer. 2024 Oct 4;12(10):e009960. doi: 10.1136/jitc-2024-009960.
BACKGROUND
Chimeric antigen receptor (CAR)-T cells face many obstacles in solid tumor therapy, including heterogeneous antigen expression and inefficient T cell persistence. Guanylyl cyclase C (GUCY2C) has been identified as a suitable tumor antigen for targeted therapy due to its intestinal-restricted expression pattern in normal tissues and steady overexpression in gastrointestinal tumors, especially colorectal cancer. An antigen-sensitive and long-lasting CAR-T cell targeting GUCY2C was investigated in this study.
METHODS
Using constructed tumor cell lines with various GUCY2C expression densities, we screened out an antigen-sensitive single chain variable fragment (scFv) that enabled CAR-T cells to efficiently eradicate the GUCY2C lowly expressed tumor cells. CAR-T cells with different compositions of the hinge, transmembrane and costimulatory domains were also constructed for selection of the long-lasting CAR-T format with durable antitumor efficacy in vitro and in tumor-bearing mice. The underlying mechanism was further investigated based on mutation of the hinge and transmembrane domains.
RESULTS
We found that the composition of the antigen-sensitive scFv, CD8α hinge, CD8α transmembrane, and CD28 costimulatory domains boosted CAR-T cells to rapidly kill tumors, maintain high expansion capacity, and long-term efficacy in various colorectal cancer models. The durable antitumor function was attributed to the optimal CAR tonic signaling that conferred CAR-T cells with autonomous activation, proliferation, survival and cytokine release in the absence of antigen stimulation. The tonic signaling was associated with the length and the cysteine residues in the CD8α hinge and transmembrane domains.
CONCLUSIONS
This study demonstrated a potent GUCY2C-targeted CAR-T cell for gastrointestinal tumor therapy and highlights the importance of adequate tonic signaling for effective CAR-T cell therapy against solid tumors.
背景
嵌合抗原受体 (CAR)-T 细胞在实体瘤治疗中面临许多障碍,包括抗原表达异质性和 T 细胞持久性差。鸟苷酸环化酶 C (GUCY2C) 因其在正常组织中肠道限制性表达模式和胃肠道肿瘤(尤其是结直肠癌)中的稳定过表达而被鉴定为靶向治疗的合适肿瘤抗原。本研究旨在研究针对 GUCY2C 的抗原敏感和持久的 CAR-T 细胞。
方法
使用具有不同 GUCY2C 表达密度的构建肿瘤细胞系,我们筛选出一种抗原敏感的单链可变片段 (scFv),使 CAR-T 细胞能够有效地清除 GUCY2C 低表达的肿瘤细胞。还构建了具有不同铰链、跨膜和共刺激结构域组成的 CAR-T 细胞,以选择在体外和荷瘤小鼠中具有持久抗肿瘤疗效的持久 CAR-T 格式。还进一步基于铰链和跨膜结构域的突变研究了潜在机制。
结果
我们发现,抗原敏感的 scFv、CD8α 铰链、CD8α 跨膜和 CD28 共刺激结构域的组成使 CAR-T 细胞能够快速杀死肿瘤,保持高扩增能力,并在各种结直肠癌模型中具有长期疗效。持久的抗肿瘤功能归因于最佳的 CAR 紧张信号,该信号赋予 CAR-T 细胞在没有抗原刺激的情况下自主激活、增殖、存活和细胞因子释放的能力。紧张信号与 CD8α 铰链和跨膜结构域的长度和半胱氨酸残基有关。
结论
本研究证明了一种有效的 GUCY2C 靶向 CAR-T 细胞用于胃肠道肿瘤治疗,并强调了适当的紧张信号对于针对实体瘤的有效 CAR-T 细胞治疗的重要性。
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