体内
转录组
下调和上调
癌症研究
嵌合抗原受体
体外
细胞毒性
基因表达谱
生物
细胞因子
细胞生物学
计算生物学
体外毒理学
免疫疗法
化学
药理学
离体
代谢组学
免疫学
免疫系统
生物信息学
外周血单个核细胞
细胞培养
效力
基因剔除小鼠
表型
细胞毒性T细胞
受体
信号转导
分泌物
胰腺癌
作者
Joseph S. Durgin,Shin H Seo,Shadab Kazmi,Bakir Valentić,Chloe Leff,Martina Markovska,Xiaoling Jin,Feng Shen,Abdulla Berjis,Nandana Mukherjee,Ashwin Sannecy,Gabriela Plesa,Khatuna Gabunia,John Scholler,Saar Gill,Roddy S. O’Connor,Carl H. June,Saba Ghassemi
出处
期刊:Blood
[Elsevier BV]
日期:2026-04-16
标识
DOI:10.1182/blood.2026033460
摘要
Chimeric antigen receptor (CAR) T-cell therapies have transformed the treatment of B-cell malignancies, yet challenges including manufacturing delays, T-cell exhaustion, and limited persistence impede broader clinical success. Here, we report the single day production of non-activated CAR T-cells engineered to secrete interleukin-18 (IL-18), a pro-inflammatory cytokine that enhances T-cell function. These non-activated CART-IL18 cells exhibit robust anti-tumor efficacy across xenograft models of lymphoma, leukemia, and pancreatic cancer. IL-18 expression enhances the functional advantages of naïve-like non-activated CAR T-cells, resulting in improved persistence, metabolic fitness, and resistance to exhaustion. Single-cell transcriptomic analysis revealed upregulation of IL7R, KLF2, and MCL1, alongside suppression of inhibitory checkpoint genes such as PDCD1, TOX, and HAVCR2. Metabolomic profiling demonstrated enhanced mitochondrial bioenergetics, with increased spare respiratory capacity and accumulation of α-ketoglutarate, malate, and spermine. Functional in vitro and in vivo profiling demonstrated enhanced per-cell cytotoxicity and in vivo durability. We complemented these studies with single-cell transcriptomic and metabolomic analyses to define CAR T-cell biological states beyond what is captured by xenograft tumor clearance. This IL-18-enhanced, activation-free CAR T product offers a clinically actionable platform with the potential to reduce vein-to-vein time while improving product potency and persistence, providing a rationale for clinical testing in patients with tumors refractory to standard CAR T.
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