磷脂酰聚糖蛋白 3 靶向嵌合抗原受体 T 细胞治疗肝细胞癌的脱落抗原诱导阻断效应。
Shed antigen-induced blocking effect on CAR-T cells targeting Glypican-3 in Hepatocellular Carcinoma.
机构信息
Key Laboratory of Human Functional Genomics of Jiangsu Province, National Health Commission Key Laboratory of Antibody Techniques, School of Basic Medical Sciences, Nanjing Medical University, Nanjing, Jiangsu, China.
Department of Nephrology, The Affiliated BenQ Hospital of Nanjing Medical University, Nanjing, Jiangsu, China.
出版信息
J Immunother Cancer. 2021 Apr;9(4). doi: 10.1136/jitc-2020-001875.
BACKGROUND
Glypican-3 (GPC3), a cell surface glycoprotein that is pathologically highly expressed in hepatocellular carcinoma (HCC), is an attractive target for immunotherapies, including chimeric antigen receptor (CAR) T cells. The serum GPC3 is frequently elevated in HCC patients due to the shedding effect of cell surface GPC3. The shed GPC3 (sGPC3) is reported to block the function of cell-surface GPC3 as a negative regulator. Therefore, it would be worth investigating the potential influence of antigen shedding in anti-GPC3 CAR-T therapy for HCC.
METHODS
In this study, we constructed two types of CAR-T cells targeting distinct epitopes of GPC3 to examine how sGPC3 influences the activation and cytotoxicity of CAR-T cells in vitro and in vivo by introducing sGPC3 positive patient serum or recombinant sGPC3 proteins into HCC cells or by using sGPC3-overexpressing HCC cell lines.
RESULTS
Both humanized YP7 CAR-T cells and 32A9 CAR-T cells showed GPC3-specific antitumor functions in vitro and in vivo. The existence of sGPC3 significantly inhibited the release of cytokines and the cytotoxicity of anti-GPC3 CAR-T cells in vitro. In animal models, mice carrying Hep3B xenograft tumors expressing sGPC3 exhibited a worse response to the treatment with CAR-T cells under both a low and high tumor burden. sGPC3 bound to CAR-T cells but failed to induce the effective activation of CAR-T cells. Therefore, sGPC3 acted as dominant negative regulators when competed with cell surface GPC3 to bind anti-GPC3 CAR-T cells, leading to an inhibitory effect on CAR-T cells in HCC.
CONCLUSIONS
We provide a proof-of-concept study demonstrating that GPC3 shedding might cause worse response to CAR-T cell treatment by competing with cell surface GPC3 for CAR-T cell binding, which revealed a new mechanism of tumor immune escape in HCC, providing a novel biomarker for patient enrolment in future clinical trials and/or treatments with GPC3-targeted CAR-T cells.
背景
磷脂酰聚糖蛋白 3(GPC3)是一种细胞表面糖蛋白,在肝细胞癌(HCC)中病理性高表达,是免疫疗法的一个有吸引力的靶点,包括嵌合抗原受体(CAR)T 细胞。由于细胞表面 GPC3 的脱落效应,HCC 患者的血清 GPC3 经常升高。据报道,脱落的 GPC3(sGPC3)作为负调节剂阻断细胞表面 GPC3 的功能。因此,研究抗原脱落对 HCC 抗 GPC3 CAR-T 治疗的潜在影响是值得的。
方法
在这项研究中,我们构建了两种针对 GPC3 不同表位的 CAR-T 细胞,通过将 sGPC3 阳性患者血清或重组 sGPC3 蛋白引入 HCC 细胞,或使用过表达 sGPC3 的 HCC 细胞系,研究 sGPC3 如何影响 CAR-T 细胞在体外和体内的激活和细胞毒性。
结果
人源化 YP7 CAR-T 细胞和 32A9 CAR-T 细胞在体外和体内均表现出 GPC3 特异性抗肿瘤功能。sGPC3 的存在显著抑制了抗 GPC3 CAR-T 细胞在体外的细胞因子释放和细胞毒性。在动物模型中,携带表达 sGPC3 的 Hep3B 异种移植肿瘤的小鼠在低肿瘤负荷和高肿瘤负荷下对 CAR-T 细胞治疗的反应均较差。sGPC3 与 CAR-T 细胞结合,但未能诱导 CAR-T 细胞的有效激活。因此,当与细胞表面 GPC3 竞争结合抗 GPC3 CAR-T 细胞时,sGPC3 作为显性负调节剂发挥作用,导致 HCC 中 CAR-T 细胞受到抑制。
结论
我们提供了一项概念验证研究,证明 GPC3 脱落可能通过与细胞表面 GPC3 竞争结合 CAR-T 细胞,导致对 CAR-T 细胞治疗的反应更差,揭示了 HCC 中肿瘤免疫逃逸的新机制,为未来临床试验中患者入组提供了新的生物标志物和/或 GPC3 靶向 CAR-T 细胞治疗。
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