Timosaponin AIII enhances CAR-T cell potency and prevents relapse through impairing CAR-Tregs
Hou Mingqi, Zhang Wenjun, Qi Ziping, Li Guiming, Mei Husheng, Qi Shuang, Jin Rui, Zhao Yuedong, Tang Xiaochen, Xiu Bing, Chen Xiaotong, Zhao Yunshuo, Hu Chen, Qian Changlin, Li Xiuchun, Xu Zhan, Chen
Journal:Nature Communications
IF:18.1
DOI:10.1038/s41467-026-70867-5
PMID:
Published:2026-03-31
research field:肿瘤学分子生物学药理学细胞生物学免疫治疗
Abstract
Chimeric antigen receptor (CAR)-T cell therapy has transformed treatment of relapsed/refractory DLBCL, yet resistance driven by regulatory T cells (Tregs) limits its efficacy. Here we identify Timosaponin AIII (TAIII), a clinical-stage natural product, as an effective modulator of CAR-T function that depletes CAR-Tregs while enhancing effector activity. Mechanistically, TAIII acts as an allosteric A2AR inhibitor by competing with cholesterol, suppressing CREB-dependent FoxP3 transcription and disrupting the A2AR-Treg axis. Ablation of A2AR or Tregs in vitro and in vivo abolishes TAIII activity, confirming specificity. Furthermore, TAIII reduces intratumoral Tregs, increases CD8⁺ T cells infiltration, and potentiates PD-1 blockade in solid tumor models. Importantly, TAIII promotes central memory T-cell formation and enhances CAR-T cytotoxic cytokine secretion. Combining or pretreating CAR-T cells with TAIII markedly improves antitumor efficacy and prevents late relapse across preclinical models. These findings establish TAIII as a combinatorial strategy to deplete CAR-Tregs, enhance CAR-T activity, and extend therapeutic durability.
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