Razavi Azadeh Sadat, Loskog Angelica, Razi Sepideh, Rezaei Nima
Cancer Immunology Project (CIP), Universal Scientific Education and Research Network (USERN), Tehran, Iran.
Department of Immunology, Genetics and Pathology, Rudbeck Laboratory, Uppsala University, Dag Hammarskjöldsväg 20, 751 85, Uppsala, Sweden.
Int Immunopharmacol. 2023 Jan;114:109593. doi: 10.1016/j.intimp.2022.109593. Epub 2022 Dec 20.
Chimeric antigen receptor (CAR) T cell therapy is introduced as an effective, rapidly evolving therapeutic to treat cancer, especially cancers derived from hematological cells, such as B cells. CAR T cell gene constructs combine a tumor-targeting device coupled to the T cell receptor (TCR) zeta chain domain with different signaling domains such as domains derived from CD28 or 4-1BB (CD137). The incorporation of each specific co-stimulatory domain targets the immunometabolic pathways of CAR T cells as well as other signaling pathways. Defining the immunometabolic and signaling pathways by which CAR T cells become and remain active, survive, and eliminate their targets may represent a huge step forward in this relatively young research field as the CAR gene can be tailored to gain optimal function also for solid tumors with elaborate immunosuppression and protective stroma. There is a close relationship between different signaling domains applied in CAR T cells, and difficult to evaluate the benefit from different tested CAR gene constructs. In this review, we attempt to collect the latest findings regarding the CAR T cell signaling pathways that affect immunometabolic pathways.
嵌合抗原受体(CAR)T细胞疗法是一种用于治疗癌症的有效且快速发展的疗法,尤其适用于治疗源自血液细胞(如B细胞)的癌症。CAR T细胞基因构建体将与T细胞受体(TCR)ζ链结构域偶联的肿瘤靶向装置与不同的信号结构域(如源自CD28或4-1BB(CD137)的结构域)相结合。每个特定共刺激结构域的整合靶向CAR T细胞的免疫代谢途径以及其他信号通路。确定CAR T细胞激活、存活并清除其靶标的免疫代谢和信号通路,可能代表着这一相对年轻的研究领域向前迈出了巨大的一步,因为CAR基因可以进行定制,以在具有复杂免疫抑制和保护性基质的实体瘤中也获得最佳功能。应用于CAR T细胞的不同信号结构域之间存在密切关系,难以评估不同测试的CAR基因构建体的益处。在本综述中,我们试图收集有关影响免疫代谢途径的CAR T细胞信号通路的最新发现。
