Antibody-based binding domain fused to TCRγ chain facilitates T cell cytotoxicity for potent anti-tumor response.

IF 5.9 2区 医学 Q1 ONCOLOGY Oncogenesis Pub Date : 2023-06-22 DOI:10.1038/s41389-023-00480-4
Zhao Chen, Changyou Lin, Hong Pei, Xiaomei Yuan, Jia Xu, Mingwei Zou, Xinyuan Zhang, Amber Fossier, Meizhu Liu, Seungah Goo, Lei Lei, Jia Yang, Catherine Novick, Jiqing Xu, Ge Ying, Zhihong Zhou, Jianbo Wu, Chunyi Tang, Wenying Zhang, Zhenping Wang, Zhihao Wang, Huitang Zhang, Wenzhong Guo, Qidong Hu, Henry Ji, Runqiang Chen
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Abstract

Chimeric antigen receptor T-cell (CAR-T) therapy has demonstrated potent clinical efficacy in the treatment of hematopoietic malignancies. However, the application of CAR-T in solid tumors has been limited due in part to the expression of inhibitory molecules in the tumor microenvironment, leading to T-cell exhaustion. To overcome this limitation, we have developed a synthetic T-cell receptor (TCR) that targets programmed death-ligand 1 (PD-L1), a molecule that is widely expressed in various solid tumors and plays a pivotal role in T-cell exhaustion. Our novel TCR platform is based on antibody-based binding domain, which is typically a single-chain variable fragment (scFv), fused to the γδ TCRs (TCRγδ). We have utilized the T-cell receptor alpha constant (TRAC) locus editing approach to express cell surface scFv of anti-PD-L1, which is fused to the constant region of the TCRγ or TCRδ chain in activated T cells derived from peripheral blood mononuclear cells (PBMCs). Our results indicate that these reconfigured receptors, both γ-TCRγδ and δ-TCRγδ, have the capability to transduce signals, produce inflammatory cytokines, degranulate and exert tumor killing activity upon engagement with PD-L1 antigen in vitro. Additionally, we have also shown that γ-TCRγδ exerted superior efficacy than δ-TCRγδ in in vivo xenograft model.

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基于抗体的结合域与TCRγ链融合,促进T细胞的细胞毒性,从而产生有效的抗肿瘤反应。
嵌合抗原受体t细胞(CAR-T)疗法在治疗造血系统恶性肿瘤中已显示出强大的临床疗效。然而,CAR-T在实体肿瘤中的应用一直受到限制,部分原因是肿瘤微环境中抑制分子的表达导致t细胞衰竭。为了克服这一限制,我们开发了一种合成的t细胞受体(TCR),其靶向程序性死亡配体1 (PD-L1), PD-L1是一种在各种实体肿瘤中广泛表达的分子,在t细胞衰竭中起关键作用。我们的新型TCR平台基于基于抗体的结合域,该结合域通常是一个单链可变片段(scFv),融合到γδ TCR (TCRγδ)中。我们利用T细胞受体α常数(TRAC)基因座编辑方法来表达细胞表面抗pd - l1的scFv,该scFv融合到来自外周血单核细胞(PBMCs)的活化T细胞的TCRγ或TCRδ链的恒定区域。我们的研究结果表明,这些重组受体γ-TCRγδ和δ-TCRγδ在体外与PD-L1抗原结合后具有信号转导、产生炎症细胞因子、脱颗粒和杀伤肿瘤活性的能力。此外,我们还发现γ-TCRγδ在体内异种移植模型中表现出比δ-TCRγδ更好的疗效。
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来源期刊
Oncogenesis
Oncogenesis ONCOLOGY-
CiteScore
11.90
自引率
0.00%
发文量
70
审稿时长
26 weeks
期刊介绍: Oncogenesis is a peer-reviewed open access online journal that publishes full-length papers, reviews, and short communications exploring the molecular basis of cancer and related phenomena. It seeks to promote diverse and integrated areas of molecular biology, cell biology, oncology, and genetics.
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