Smirnov Sergei, Zaritsky Yuriy, Silonov Sergey, Gavrilova Anastasia, Fonin Alexander
Institute of Cytology of the Russian Academy of Sciences, Tikhoretsky Ave. 4, St. Petersburg 194064, Russia.
Biomolecules. 2025 Oct 2;15(10):1407. doi: 10.3390/biom15101407.
Therapy with chimeric antigen receptor (CAR)-T cells has revolutionized the treatment of hematological malignancies. However, their application in solid tumors remains a formidable challenge due to obstacles such as the immunosuppressive tumor microenvironment, tumor heterogeneity, and limited T cell persistence. Although second- and third-generation CAR-T cells have shown restricted efficacy in clinical trials, next-generation strategies-including cytokine-armored CAR-T cells (e.g., IL-15, IL-7/CCL19), logic-gated systems, and localized delivery approaches-demonstrate promising potential to overcome these limitations. This review examines the major barriers impeding CAR-T cell efficacy in solid tumors, evaluates clinical outcomes from conventional CAR constructs, and highlights innovative strategies being tested in recent clinical trials. Key advances discussed include the use of dominant-negative receptors (e.g., TGFβRII) to combat immunosuppression and the co-expression of bispecific T cell engagers (BiTEs) to address antigen escape.
嵌合抗原受体(CAR)-T细胞疗法彻底改变了血液系统恶性肿瘤的治疗方式。然而,由于免疫抑制性肿瘤微环境、肿瘤异质性和T细胞持久性有限等障碍,它们在实体瘤中的应用仍然是一项艰巨的挑战。尽管第二代和第三代CAR-T细胞在临床试验中显示出有限的疗效,但包括细胞因子增强型CAR-T细胞(如IL-15、IL-7/CCL19)、逻辑门控系统和局部递送方法在内的下一代策略,显示出克服这些限制的有前景的潜力。这篇综述探讨了阻碍CAR-T细胞在实体瘤中发挥疗效的主要障碍,评估了传统CAR构建体的临床结果,并强调了近期临床试验中正在测试的创新策略。讨论的关键进展包括使用显性负性受体(如TGFβRII)来对抗免疫抑制,以及共表达双特异性T细胞衔接器(BiTEs)来解决抗原逃逸问题。
