JAK-STAT激活的、抗自相残杀的靶向膜结合肿瘤坏死因子的嵌合抗原受体T细胞可有效治疗急性髓系白血病和实体瘤。

JAK-STAT-activated, fratricide-resistant CAR-T cells targeting membrane-bound TNF effectively treat AML and solid tumors.

作者信息

Nakashima Takahiro, Ouchida Tsunenori, Ishikawa Yuichi, Ito Yusuke, Hayakawa Taeko, Yoshikawa Toshiaki, Zhang Haosong, Kasuya Hitomi, Li Yang, Matsukawa Tetsuya, Inoue Satoshi, Iida Shinsuke, Kiyoi Hitoshi, Kagoya Yuki

机构信息

Division of Tumor Immunology, Institute for Advanced Medical Research, Keio University School of Medicine, Tokyo, Japan.

Division of Immune Response, Aichi Cancer Center Research Institute, Nagoya, Japan.

出版信息

J Immunother Cancer. 2025 Jul 13;13(7):e011067. doi: 10.1136/jitc-2024-011067.

DOI:10.1136/jitc-2024-011067

PMID:40659447

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC12258316/

Abstract

BACKGROUND

While chimeric antigen receptor (CAR)-T cell therapy exhibits a robust therapeutic efficacy against B-cell malignancies and multiple myeloma, its efficacy and safety have not been established for acute myeloid leukemia (AML) and solid tumors due to the paucity of established target antigens. Some AML and solid tumor cells express tumor necrosis factor (TNF), which is initially expressed on the cell surface prior to shedding.

METHODS

In this study, we obtained monoclonal antibodies against the N-terminal fragment of TNF (TNF-NTF) that remains on the cell surface after shedding. We then generated CAR-T cells to target TNF-NTF using the antibody sequence. To enhance the therapeutic efficacy of TNF-NTF CAR-T cells, we further engineered the previously developed chimeric cytokine receptor consisting of GP130, IL6R, and constitutively active IL7R with the M452L mutation (G6/7R).

RESULTS

TNF-NTF CAR-T cells efficiently lysed TNF-expressing leukemia cells , while showing limited antitumor efficacy due to poor expansion and persistence. Activated T cells upregulate TNF, which was recognized by TNF-NTF CAR-T cells and led to fratricide. Genetic knockout (KO) of significantly enhanced the viability and proliferation of TNF-NTF CAR-T cells, while slightly reducing their cytotoxic activity. In addition, ectopic expression of G6/7R improved the effector function of TNF-NTF CAR-T cells through constitutive activation of janus kinase (JAK)-signal transducers and activators of transcription (STAT) signaling. The G6/7R-expressing -KO TNF-NTF CAR-T cells exhibited superior persistence and durable antileukemic efficacy compared with parental CAR-T cells. We also confirmed that TNF-NTF CAR-T cells can target primary AML cells, including a leukemia-initiating population with colony-forming capacity. Unlike CD33, targeting TNF-NTF did not show cytotoxicity against normal hematopoietic stem/progenitor cells. Finally, we demonstrated the curative efficacy of G6/7R -KO TNF-NTF CAR-T cells against TNF-expressing ovarian tumor cells .

CONCLUSIONS

Our studies highlight TNF-NTF as a promising cell surface target for CAR-T cell therapy that can be applied to AML as well as solid tumors.

摘要

背景

嵌合抗原受体（CAR）-T细胞疗法对B细胞恶性肿瘤和多发性骨髓瘤显示出强大的治疗效果，但由于缺乏已确定的靶抗原，其对急性髓系白血病（AML）和实体瘤的疗效及安全性尚未确定。一些AML和实体瘤细胞表达肿瘤坏死因子（TNF），该因子在脱落前最初表达于细胞表面。

方法

在本研究中，我们获得了针对TNF脱落后仍保留在细胞表面的N端片段（TNF-NTF）的单克隆抗体。然后，我们利用该抗体序列生成靶向TNF-NTF的CAR-T细胞。为增强TNF-NTF CAR-T细胞的治疗效果，我们进一步构建了先前开发的由GP130、IL6R和具有M452L突变的组成型活性IL7R（G6/7R）组成的嵌合细胞因子受体。

结果

TNF-NTF CAR-T细胞能有效裂解表达TNF的白血病细胞，但由于扩增和持久性较差，抗肿瘤效果有限。活化的T细胞会上调TNF，而TNF-NTF CAR-T细胞可识别TNF，从而导致自相残杀。基因敲除（KO）显著提高了TNF-NTF CAR-T细胞的活力和增殖能力，同时略微降低了它们的细胞毒性活性。此外，G6/7R的异位表达通过组成型激活janus激酶（JAK）-信号转导子和转录激活子（STAT）信号通路，改善了TNF-NTF CAR-T细胞的效应功能。与亲本CAR-T细胞相比，表达G6/7R的KO TNF-NTF CAR-T细胞表现出更好的持久性和持久的抗白血病疗效。我们还证实，TNF-NTF CAR-T细胞可靶向原发性AML细胞，包括具有集落形成能力的白血病起始群体。与CD33不同，靶向TNF-NTF对正常造血干/祖细胞没有细胞毒性。最后，我们证明了G6/7R KO TNF-NTF CAR-T细胞对表达TNF的卵巢肿瘤细胞具有治愈效果。