以 GD2 和 GPC2 为靶点的嵌合抗原受体 T 细胞增强了高危神经母细胞瘤的抗肿瘤活性。

IF 3.7 3区医学 Q2 BIOTECHNOLOGY & APPLIED MICROBIOLOGY

Cytotherapy Pub Date : 2024-05-31 DOI:10.1016/j.jcyt.2024.05.023

Huantong Wu, Guangji Zhang, Zhongfeng Liu, Weihua Liu, Xuan Wang, Yu Zhao

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引用次数: 0

摘要

背景目的：针对单一抗原的嵌合抗原受体 T（CAR-T）细胞对实体瘤的活性有限，原因是 T 细胞持久性差、浸润效率低、衰竭以及肿瘤相关抗原（TAA）表达不均。高危神经母细胞瘤（HRNB）也是如此，这是一种致命的小儿颅外恶性肿瘤。为了克服这些障碍，我们开发了一种使用GD2特异性和GPC2特异性CAR-T细胞的组合策略，以提高免疫治疗效果：我们分别开发了含有选择性结构域（sCAR）的GD2特异性和GPC2特异性CAR，该选择性结构域是由10个氨基酸组成的多肽，来源于人类核自身抗原La/SS-B。通过选择性结构域特异性单克隆抗体（SmAb）刺激 sCAR 接种的 T 细胞，这些构建物使我们能够生成两种不同的 HRNB 抗原特异性 CAR-T 细胞，并增强其生物活性。在表达不同TAA水平的神经母细胞瘤细胞系中，测定了SmAb对GD2-和GPC2-特异性sCAR的结合亲和力和刺激作用，并量化了GD2sCAR-T和GPC2sCAR-T细胞的瞬时和持续抗肿瘤细胞毒性。在体外和体内评估了单个或组合 sCAR-T 细胞介导的抗肿瘤药物效应和细胞机制：结果：GD2-和GPC2-特异性sCAR与亲本具有相似的抗原特异性结合亲和力，并能被SmAb识别。SmAb 介导的刺激可选择性地激活 sCAR-T 增殖，并增加最终产物中的中枢记忆 T 细胞。SmAb刺激的sCAR-T细胞具有更强的瞬时细胞溶解活性，联合疗法可通过释放TNF-α和IL-15延长体外长期抗肿瘤活性。受刺激的sCAR-T细胞能克服HRNB中的异质性抗原表达，多TAA靶向策略在体内尤其有效，能通过caspase-3/PARP途径诱导细胞凋亡，并抑制多种促瘤细胞因子的释放：这些数据表明，联合靶向多种TAAs是克服实体瘤异源抗原表达和延长CAR-T细胞持久性以进行HRNB免疫治疗的一种有前途的策略。

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Enhanced anti-tumor activity mediated by combination chimeric antigen receptor T cells targeting GD2 and GPC2 in high-risk neuroblastoma.

Background aims: Chimeric antigen receptor T (CAR-T) cells targeting single antigens show limited activity against solid tumors due to poor T cell persistence, low efficiency infiltration, and exhaustion together with heterogeneous tumor-associated antigen (TAA) expression. This is also true in high-risk neuroblastoma (HRNB), a lethal pediatric extracranial malignancy. To overcome these obstacles, a combinational strategy using GD2-specific and GPC2-specific CAR-T cells was developed to improve immunotherapeutic efficacy.

Methods: We individually developed GD2-specific and GPC2-specific CARs containing a selective domain (sCAR) which was a peptide of 10 amino acids derived from human nuclear autoantigen La/SS-B. These constructs allowed us to generate two different HRNB antigen-specific CAR-T cells with enhanced biological activity through stimulating sCAR-engrafted T cells via a selective domain-specific monoclonal antibody (SmAb). Binding affinity and stimulation of GD2- and GPC2-specific sCARs by SmAb were measured, and transient and persistent anti-tumor cytotoxicity of GD2sCAR-T and GPC2sCAR-T cells were quantified in neuroblastoma cell lines expressing different TAA levels. The anti-tumor pharmaceutical effects and cellular mechanisms mediated by single or combinational sCAR-T cells were evaluated in vitro and in vivo.

Results: GD2- and GPC2-specific sCARs had antigen-specific binding affinity similar to their parental counterparts and were recognized by SmAb. SmAb-mediated stimulation selectively activated sCAR-T proliferation and increased central memory T cells in the final products. SmAb-stimulated sCAR-T cells had enhanced transient cytolytic activity, and combination therapy extended long-term anti-tumor activity in vitro through TNF-α and IL-15 release. Stimulated sCAR-T cells overcame heterogeneous antigen expression in HRNB, and the multi-TAA-targeting strategy was especially efficacious in vivo, inducing apoptosis through the caspase-3/PARP pathway and inhibiting the release of several tumor-promoting cytokines.

Conclusions: These data suggest that combined targeting of multiple TAAs is a promising strategy to overcome heterogenous antigen expression in solid tumors and extend CAR-T cell persistence for HRNB immunotherapy.

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来源期刊

Cytotherapy 医学-生物工程与应用微生物

CiteScore

6.30

自引率

4.40%

发文量

683

审稿时长

49 days

期刊介绍： The journal brings readers the latest developments in the fast moving field of cellular therapy in man. This includes cell therapy for cancer, immune disorders, inherited diseases, tissue repair and regenerative medicine. The journal covers the science, translational development and treatment with variety of cell types including hematopoietic stem cells, immune cells (dendritic cells, NK, cells, T cells, antigen presenting cells) mesenchymal stromal cells, adipose cells, nerve, muscle, vascular and endothelial cells, and induced pluripotential stem cells. We also welcome manuscripts on subcellular derivatives such as exosomes. A specific focus is on translational research that brings cell therapy to the clinic. Cytotherapy publishes original papers, reviews, position papers editorials, commentaries and letters to the editor. We welcome "Protocols in Cytotherapy" bringing standard operating procedure for production specific cell types for clinical use within the reach of the readership.