Microenvironment-responsive anti-PD-L1 × CD3 bispecific T-cell engager for solid tumor immunotherapy

免疫疗法 肿瘤微环境 癌症研究 化学 癌症免疫疗法 T细胞 CD3型 分子生物学 免疫系统 生物 免疫学 CD8型 肿瘤细胞
作者
Dingkang Liu,Lichen Bao,Haichao Zhu,Yali Yue,Tian Jing,Xiangdong Gao,Jun Yin
出处
期刊:Journal of Controlled Release [Elsevier]
卷期号:354: 606-614 被引量:6
标识
DOI:10.1016/j.jconrel.2023.01.041
摘要

Bispecific T-cell Engager (BiTE) antibodies can redirect T-cells to tumor cells, and turn on the targeted lysis of tumor cells. However, BiTE has been challenging in solid tumors due to short plasma half-life, “off-target” effect, and immunosuppression via PD-1/PD-L1 axis. This study designed a safe, long-acting, and highly effective Protease-Activated PSTAGylated BiTE, named PAPB, which includes a shielding polypeptide domain (PSTAG), a protease-activated linker, and a BiTE core. The BiTE core consists of two scFvs targeting PD-L1 and CD3. BiTE core bound PD-L1 and CD3 in a dose-dependent manner, and PAPB can release BiTE core in response to MMP2 in the tumor microenvironment to exert antitumor activity. The plasma half-life of PAPB in mice was significantly prolonged from 2.46 h to 6.34 h of the BiTE core. In mice bearing melanoma (A375) xenografts, PAPB significantly increased infiltration of T lymphocytes in tumor tissue, and inhibited tumor proliferation without activating T-cells in the peripheral blood. Overall, the engineering protein PAPB could be a promising drug candidate for solid tumor immunotherapy.
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