用PD1-TIGIT嵌合免疫检查点开关受体增强T细胞抗肿瘤功效。

IF 7.2 2区 医学 Oncoimmunology Pub Date : 2023-10-05 eCollection Date: 2023-01-01 DOI:10.1080/2162402X.2023.2265703
Jingjing Zhao, Jiebin Dong, Changwen Deng, Qianjing Zhang, Shicheng Sun, Honggang Li, Yun Bai, Hongkui Deng
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摘要

嵌合抗原受体(CAR)T细胞免疫疗法在治疗血液系统恶性肿瘤方面取得了成功;然而,它在实体瘤中的疗效和应用仍然有限。免疫抑制因子,特别是抑制性检查点分子,限制实体瘤内CAR T细胞的活性。检查点通路的调节已成为促进CAR T细胞抗肿瘤反应的一种有前途的方法。程序性细胞死亡蛋白1(PD1)和具有Ig和ITIM结构域的T细胞免疫受体(TIGIT)是抑制T细胞抗肿瘤活性的两种关键免疫检查点分子。同时靶向这两种抑制分子可能是一种有效的检查点调节策略。在这里,我们开发了一种PD1-TIGIT嵌合免疫检查点开关受体(CISR),它通过逆转PD1/PDL1和/或TIGIT/CD155的抑制性检查点信号来增强CAR T细胞免疫疗法的疗效。除了中和PDL1和CD155外,这种嵌合受体还通过CD28的跨膜区和细胞内结构域进行工程设计,从而有效增强T细胞存活和肿瘤靶向功能。值得注意的是,在PDL1和CD155的同时刺激下,与传统CAR T细胞相比,CISR-CAR T电池在细胞存活、增殖、细胞因子释放和体外细胞毒性方面表现出优异的性能。利用细胞系和患者来源的异种移植肿瘤模型的实验表明,CISR-CAR T细胞在体内表现出强大的浸润和抗肿瘤效率。我们的研究结果强调了CISR策略增强T细胞抗肿瘤疗效的潜力,并为基于T细胞的免疫治疗提供了一种替代方法。
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Enhancing T cell anti-tumor efficacy with a PD1-TIGIT chimeric immune-checkpoint switch receptor.

Chimeric antigen receptor (CAR) T cell immunotherapy has demonstrated success in the treatment of hematological malignancies; however, its efficacy and applications in solid tumors remain limited. Immunosuppressive factors, particularly inhibitory checkpoint molecules, restrict CAR T cell activity inside solid tumors. The modulation of checkpoint pathways has emerged as a promising approach to promote anti-tumor responses in CAR T cells. Programmed cell death protein 1 (PD1) and T cell immunoreceptor with Ig and ITIM domains (TIGIT) are two critical immune-checkpoint molecules that suppress anti-tumor activity in T cells. Simultaneous targeting of these two inhibitory molecules could be an efficient checkpoint modulation strategy. Here, we developed a PD1-TIGIT chimeric immune-checkpoint switch receptor (CISR) that enhances the efficacy of CAR T cell immunotherapy by reversing the inhibitory checkpoint signals of PD1/PDL1 and/or TIGIT/CD155. In addition to neutralizing PDL1 and CD155, this chimeric receptor is engineered with the transmembrane region and intracellular domain of CD28, thereby effectively enhancing T cell survival and tumor-targeting functions. Notably, under simultaneous stimulation of PDL1 and CD155, CISR-CAR T cells demonstrate superior performance in terms of cell survival, proliferation, cytokine release, and cytotoxicity in vitro, compared with conventional CAR T cells. Experiments utilizing both cell line- and patient-derived xenotransplantation tumor models showed that CISR-CAR T cells exhibit robust infiltration and anti-tumor efficiency in vivo. Our results highlight the potential for the CISR strategy to enhance T cell anti-tumor efficacy and provide an alternative approach for T cell-based immunotherapies.

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来源期刊
Oncoimmunology
Oncoimmunology ONCOLOGY-IMMUNOLOGY
CiteScore
12.80
自引率
2.80%
发文量
276
期刊介绍: Tumor immunology explores the natural and therapy-induced recognition of cancers, along with the complex interplay between oncogenesis, inflammation, and immunosurveillance. In response to recent advancements, a new journal, OncoImmunology, is being launched to specifically address tumor immunology. The field has seen significant progress with the clinical demonstration and FDA approval of anticancer immunotherapies. There's also growing evidence suggesting that many current chemotherapeutic agents rely on immune effectors for their efficacy. While oncologists have historically utilized chemotherapeutic and radiotherapeutic regimens successfully, they may have unwittingly leveraged the immune system's ability to recognize tumor-specific antigens and control cancer growth. Consequently, immunological biomarkers are increasingly crucial for cancer prognosis and predicting chemotherapy efficacy. There's strong support for combining conventional anticancer therapies with immunotherapies. OncoImmunology will welcome high-profile submissions spanning fundamental, translational, and clinical aspects of tumor immunology, including solid and hematological cancers, inflammation, and both innate and acquired immune responses.
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