Neoepitope BTLA^P267L-specific TCR-T cell immunotherapy unlocks precision treatment for hepatocellular carcinoma.

IF 5.6 2区医学 Q1 MEDICINE, RESEARCH & EXPERIMENTAL

Cancer Biology & Medicine Pub Date : 2025-04-09 DOI:10.20892/j.issn.2095-3941.2024.0434

Fang Liu, Hua Chen, Suxin Wu, Chenlu Zhu, Mingji Zhang, Wei Rui, Dong Zhou, Yang Wang, Xin Lin, Xueqiang Zhao, Yunbin Ye

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引用次数: 0

Abstract

Objective: The high heterogeneity of hepatocellular carcinoma (HCC) renders traditional therapies unable to effectively activate the patient's immune system to combat tumors. Patients with advanced HCC and T cell functional deficiencies may benefit more from cellular immunotherapy, especially tumor neoepitope-targeted T cell receptor (TCR)-T cells. Neoepitopes with strong immunogenicity provide precise targets for HCC, further enhancing the efficacy of cellular immunotherapy.

Methods: A scalable workflow for identifying neoepitopes from 7 HLA-A*02:01-restricted patients with HCC was established based on whole exome sequencing and bioinformatics analyses, followed by identification of neoepitope-specific TCRs through tetramer-based screening and single-cell TCR cloning technology, which were further validated in the JC4 cell model. The cytotoxicity of CD8⁺ TCR-T cells was evaluated in neoepitope-positive tumor cell lines or NCG mice.

Results: Ten specific neoepitopes were identified, among which neoepitope B and T lymphocyte attenuator^P267L [BTLA^P267L (SLNHSVIGL)] exhibited advantageous properties as a potential tumor target. Three TCRs (85-3, 126-5, and 52-3) were confirmed to specifically recognize the neoepitope BTLA^P267L, while no cross-recognition of irrelevant or wild-type epitopes was observed. Activated BTLA^P267L-specific CD8⁺ TCR-T cells released extensive perforin, granzyme B, IFN-γ, and TNF-α in vitro, thereby inducing strong cytotoxic effects against BTLA^P267L-positive T2 or HCC cell lines. BTLA^P267L-specific CD8⁺ TCR-T cells mediated robust tumor regression due to long-lasting survival and released perforin without causing significant cytotoxic effects on normal organs in murine experiments.

Conclusions: This preclinical study demonstrated the beneficial effects of neoepitope BTLA^P267L-specific TCR-T cell immunotherapy, unlocking a novel strategy for personalized precision therapy in HCC.

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新表位btlap267l特异性TCR-T细胞免疫疗法开启了肝癌的精准治疗。

目的：肝细胞癌（HCC）的高度异质性使得传统疗法无法有效激活患者的免疫系统来对抗肿瘤。晚期HCC和T细胞功能缺陷患者可能从细胞免疫治疗中获益更多，特别是肿瘤新表位靶向T细胞受体(TCR)-T细胞。具有较强免疫原性的新表位为HCC提供了精确的靶点，进一步提高了细胞免疫治疗的疗效。方法：基于全外显子组测序和生物信息学分析，建立了7例HLA-A*02:01限制性HCC患者新表位鉴定的可扩展工作流程，然后通过基于四聚体的筛选和单细胞TCR克隆技术鉴定新表位特异性TCR，并在JC4细胞模型中进一步验证。研究了CD8+ TCR-T细胞在新表位阳性肿瘤细胞系和NCG小鼠中的细胞毒性。结果：共鉴定出10个特异性新表位，其中新表位B和T淋巴细胞衰减因子p267l [BTLAP267L (SLNHSVIGL)]表现出作为潜在肿瘤靶点的优势特性。3个tcr（85-3、126-5和52-3）被证实特异性识别新表位BTLAP267L，而未观察到不相关或野生型表位的交叉识别。激活的btlap267l特异性CD8+ TCR-T细胞在体外释放大量穿孔素、颗粒酶B、IFN-γ和TNF-α，从而诱导对btlap267l阳性T2或HCC细胞系的强细胞毒作用。在小鼠实验中，btlap267l特异性CD8+ TCR-T细胞由于存活时间长而介导了肿瘤的稳健消退，并释放穿孔素，而不会对正常器官产生明显的细胞毒性作用。结论：这项临床前研究证明了新表位btlap267l特异性TCR-T细胞免疫治疗的有益作用，为HCC的个性化精确治疗开辟了一种新的策略。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Cancer Biology & Medicine Medicine-Oncology

CiteScore

9.80

自引率

3.60%

发文量

1143

审稿时长

12 weeks

期刊介绍： Cancer Biology & Medicine (ISSN 2095-3941) is a peer-reviewed open-access journal of Chinese Anti-cancer Association (CACA), which is the leading professional society of oncology in China. The journal quarterly provides innovative and significant information on biological basis of cancer, cancer microenvironment, translational cancer research, and all aspects of clinical cancer research. The journal also publishes significant perspectives on indigenous cancer types in China.