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靶向CD155及其受体的药物研究进展
引用本文:郑学敏,李桂霞,郝瑞家,刘艳菊,韩进,王根辈,李剑.靶向CD155及其受体的药物研究进展[J].现代药物与临床,2022,37(9):2160-2166.
作者姓名:郑学敏  李桂霞  郝瑞家  刘艳菊  韩进  王根辈  李剑
作者单位:天士力生物医药股份有限公司, 天津 300410
基金项目:湖北省科技支撑计划项目(2015BCA316)
摘    要:分化簇155(CD155)是一种单次跨膜的细胞表面蛋白,在正常组织中表达量很少或不表达,但在包括胰腺癌、胆管癌、结直肠癌、非小细胞肺癌、膀胱癌、乳腺癌的多种恶性肿瘤中高表达,使其能够成为抗肿瘤药物的理想靶点。CD155作为细胞黏附分子参与肿瘤细胞的黏附、迁移和极化,还作为免疫调节分子与T细胞或NK细胞上的包括TIGIT、DNAM-1、CD96的共刺激或共抑制受体相互作用,发挥免疫调节作用,影响免疫微环境。目前靶向CD155及其受体的药物研发火热,其高亲和力受体TITIG有多种药物进入III期临床,直接靶向CD155及其受体DNAM-1和CD96的肿瘤治疗也逐渐增加。通过对靶向CD155及其受体的药物研究进展进行综述,以期为后续的药物研发提供依据。

关 键 词:分化簇155  受体  DNAM-1  TIGIT  CD96  肿瘤
收稿时间:2022/6/29 0:00:00

Research progress on drugs targeting CD155 and its receptor
ZHENG Xue-min,LI Gui-xi,HAO Rui-ji,LIU Yan-ju,HAN Jin,WANG Gen-bei,LI Jian.Research progress on drugs targeting CD155 and its receptor[J].Drugs & Clinic,2022,37(9):2160-2166.
Authors:ZHENG Xue-min  LI Gui-xi  HAO Rui-ji  LIU Yan-ju  HAN Jin  WANG Gen-bei  LI Jian
Institution:Tasly Biopharma Co., Ltd, Tianjin 300410, China
Abstract:Cluster of differentiation 155 (CD155) is a single-pass transmembrane cell surface protein with little or no expression in normal tissues, but in pancreatic cancer, cholangiocarcinoma, colorectal cancer, non-small cell lung cancer, bladder cancer and breast cancer. It is highly expressed in various malignant tumors of breast cancer, which makes it as an ideal target for anti-tumor drugs. As a cell adhesion molecule, CD155 participates in the adhesion, migration, and polarization of tumor cells. It also acts as an immunoregulatory molecule and interacts with costimulatory or costinhibitory receptors on T cells or NK cells, including TIGIT, DNAM-1, and CD96, which regulates and affects the immune microenvironment. At present, the research and development of drugs targeting CD155 and its receptors is hot, and its high-affinity receptor TITIG has a variety of drugs entering Phase III clinical trials, and tumor treatments that directly target CD155 and its receptors DNAM-1 and CD96 are also gradually increasing. This article reviews research progress of drugs targeting CD155 and its receptors, in order to provide a basis for subsequent drug development.
Keywords:CD155  receptor  DNAM-1  TIGIT  CD96  tumor
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