Locally secreted BiTEs complement CAR T cells by enhancing killing of antigen heterogeneous solid tumors

局部分泌的 BiTE 通过增强对抗原异质性实体肿瘤的杀伤来补充 CAR-T 细胞

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作者:Yibo Yin, Jesse L Rodriguez, Nannan Li, Radhika Thokala, MacLean P Nasrallah, Li Hu, Logan Zhang, Jiasi Vicky Zhang, Meghan T Logun, Devneet Kainth, Leila Haddad, Yang Zhao, Tong Wu, Emily X Johns, Yu Long, Hongsheng Liang, Jiping Qi, Xiangtong Zhang, Zev A Binder, Zhiguo Lin, Donald M O'Rourke

Abstract

Bispecific T cell engagers (BiTEs) are bispecific antibodies that redirect T cells to target antigen-expressing tumors. We hypothesized that BiTE-secreting T cells could be a valuable therapy in solid tumors, with distinct properties in mono- or multi-valent strategies incorporating chimeric antigen receptor (CAR) T cells. Glioblastomas represent a good model for solid tumor heterogeneity, representing a significant therapeutic challenge. We detected expression of tumor-associated epidermal growth factor receptor (EGFR), EGFR variant III, and interleukin-13 receptor alpha 2 (IL13Rα2) on glioma tissues and cancer stem cells. These antigens formed the basis of a multivalent approach, using a conformation-specific tumor-related EGFR targeting antibody (806) and Hu08, an IL13Rα2-targeting antibody, as the single chain variable fragments to generate new BiTE molecules. Compared with CAR T cells, BiTE T cells demonstrated prominent activation, cytokine production, and cytotoxicity in response to target-positive gliomas. Superior response activity was also demonstrated in BiTE-secreting bivalent T cells compared with bivalent CAR T cells in a glioma mouse model at early phase, but not in the long term. In summary, BiTEs secreted by mono- or multi-valent T cells have potent anti-tumor activity in vitro and in vivo with significant sensitivity and specificity, demonstrating a promising strategy in solid tumor therapy.

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