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Disulfide-directed multicyclic peptides for chimeric antigen receptors targeting solid tumors

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作者

    Xiaoting Meng,  Keke Fu,  Yawei Liu,  Yuan Liu,  Joe Zhang,  Xi Kang,  Chuanliu Wu,  Yu-Hsuan Tsai
    Yu-Hsuan Tsai
分类
关键词
CAR T; cyclic peptide; on-target, off-tumor toxicity; cytokine release syndrome; chimeric antigen receptor; disulfide-directed multicyclic peptide (DDMP)

摘要

The clinical application of chimeric antigen receptor (CAR) T cell therapy in solid tumors remains limited due to significant safety concerns, particularly “on-target, off-tumor” toxicity and cytokine release syndrome (CRS). Here, we describe a class of CARs that employ disulfide-directed multicyclic peptides (DDMPs) as compact antigen-recognition domains targeting the tumor-associated antigens HER2 and TROP2. DDMP-based CAR T cells exhibited antigen density-dependent cytotoxicity in vitro and in vivo, efficiently eliminating cells with high antigen expression while sparing cells with low antigen levels, thereby mitigating on-target, off-tumor toxicity. In addition, DDMP-based CAR T cells secreted markedly lower levels of pro-inflammatory cytokines upon targeted killing, reducing the CRS risk. Mechanistic analyses revealed that this favorable combination of restrained cytokine release and density-gated killing is associated with distinct T cell signaling pathway engagement and reduced cell avidity relative to conventional single-chain variable fragment (scFv)-based CAR T cells. Collectively, these findings establish DDMP-based CARs as a promising framework for engineering safer, yet efficacious, CAR T therapies for solid tumors.

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已发布

2025-11-25

如何引用

Meng, X., Fu, K., Liu, Y., Liu, Y., Zhang, J., Kang, X., Wu, C., & Tsai, Y.-H. (2025). Disulfide-directed multicyclic peptides for chimeric antigen receptors targeting solid tumors. 浪淘沙预印本平台. https://doi.org/10.65215/6apa6c74

利益冲突声明

所有需要披露的利益冲突细节如下:

XM, XK, CW and YHT are inventors of a Chinese patent application related to this work.