Université Côte d'Azur, INSERM, C3M, 06204, Nice, France.
Equipe Labellisée Ligue Contre Le Cancer, 06204, Nice, France.
J Exp Clin Cancer Res. 2024 Sep 14;43(1):262. doi: 10.1186/s13046-024-03179-5.
For angioimmunoblastic T cell lymphoma (AITL), a rare cancer, no specific treatments are available and survival outcome is poor. We previously developed a murine model for AITL that mimics closely human disease and allows to evaluate new treatments. As in human AITL, the murine CD4 follicular helper T (Tfh) cells are drivers of the malignancy. Therefore, chimeric antigen receptor (CAR) T cell therapy might represent a new therapeutic option.
To prevent fratricide among CAR T cells when delivering an CD4-specific CAR, we used a lentiviral vector (LV) encoding an anti-CD4 CAR, allowing exclusive entry into CD8 T cells.
These anti-CD4CAR CD8-targeted LVs achieved in murine AITL biopsies high CAR-expression levels in CD8 T cells. Malignant CD4 Tfh cells were eliminated from the mAITL lymphoma, while the CAR + CD8 T cells expanded upon encounter with the CD4 receptor and were shaped into functional cytotoxic cells. Finally, in vivo injection of the CAR + CD8-LVs into our preclinical AITL mouse model carrying lymphomas, significantly prolonged mice survival. Moreover, the in vivo generated functional CAR + CD8 T cells efficiently reduced neoplastic T cell numbers in the mAITL tumors.
This is the first description of in vivo generated CAR T cells for therapy of a T cell lymphoma. The strategy described offers a new therapeutic concept for patients suffering from CD4-driven T cell lymphomas.
血管免疫母细胞性 T 细胞淋巴瘤(AITL)是一种罕见的癌症,目前尚无特异性治疗方法,生存预后较差。我们之前开发了一种模拟人类疾病的 AITL 小鼠模型,可用于评估新的治疗方法。与人类 AITL 一样,小鼠的 CD4 滤泡辅助 T(Tfh)细胞是恶性肿瘤的驱动因素。因此,嵌合抗原受体(CAR)T 细胞疗法可能代表一种新的治疗选择。
为了防止在递送 CD4 特异性 CAR 时 CAR-T 细胞自相残杀,我们使用了一种编码抗 CD4 CAR 的慢病毒载体(LV),允许其仅进入 CD8 T 细胞。
这些抗 CD4CAR-CD8 靶向 LV 在小鼠 AITL 活检中实现了 CD8 T 细胞中高 CAR 表达水平。恶性 CD4 Tfh 细胞从 mAITL 淋巴瘤中被消除,而 CAR+CD8 T 细胞在遇到 CD4 受体后扩增,并被塑造成功能性细胞毒性细胞。最后,将 CAR+CD8-LV 体内注射到携带淋巴瘤的临床前 AITL 小鼠模型中,显著延长了小鼠的生存时间。此外,体内生成的功能性 CAR+CD8 T 细胞有效地减少了 mAITL 肿瘤中肿瘤性 T 细胞的数量。
这是首次描述用于治疗 T 细胞淋巴瘤的体内生成的 CAR-T 细胞。所描述的策略为患有 CD4 驱动的 T 细胞淋巴瘤的患者提供了一种新的治疗概念。
