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T Lymphocytes Expressing the Switchable Chimeric Fc Receptor CD64 Exhibit Augmented Persistence and Antitumor Activity

Overview
Journal Cell Rep
Publisher Cell Press
Specialties Biology
Cell Biology
Molecular Biology
Date 2023 Jul 12
PMID 37436890
Authors
Yuanbin Cui
Tingjie Yuan
Ying Wang
Diwei Zheng
Le Qin
Shanglin Li
Zhiwu Jiang
Shouheng Lin
Wenjing Guo
Zhi Wang
Zhaoduan Liang
Yi Li
Yao Yao
Xingguo Liu
Qiannan Tang
Hai-Yan Tu
Xu-Chao Zhang
Zhaoyang Tang
Nathalie Wong
Zhenfeng Zhang
Dajiang Qin
Jean Paul Thiery
Kailin Xu
Peng Li
Affiliations
Soon will be listed here.
Abstract

Chimeric antigen receptor (CAR) T cell therapy lacks persistent efficacy with "on-target, off-tumor" toxicities for treating solid tumors. Thus, an antibody-guided switchable CAR vector, the chimeric Fc receptor CD64 (CFR64), composed of a CD64 extracellular domain, is designed. T cells expressing CFR64 exert more robust cytotoxicity against cancer cells than CFR T cells with high-affinity CD16 variant (CD16v) or CD32A as their extracellular domains. CFR64 T cells also exhibit better long-term cytotoxicity and resistance to T cell exhaustion compared with conventional CAR T cells. With trastuzumab, the immunological synapse (IS) established by CFR64 is more stable with lower intensity induction of downstream signaling than anti-HER2 CAR T cells. Moreover, CFR64 T cells exhibit fused mitochondria in response to stimulation, while CARH2 T cells contain predominantly punctate mitochondria. These results show that CFR64 T cells may serve as a controllable engineered T cell therapy with prolonged persistence and long-term antitumor activity.

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