Mesothelin CAR T-cells secreting anti-FAP/anti-CD3 molecules efficiently target pancreatic adenocarcinoma and its stroma

基质 腺癌 癌症研究 胰腺癌 间皮素 生物 病理 医学 癌症 抗原 免疫学 免疫组织化学 遗传学
作者
Marc Wehrli,Samantha Guinn,Filippo Birocchi,Adam Kuo,Yi Sun,Rebecca C. Larson,Amaya Jimeno Almazán,Irene Scarfò,Amanda A. Bouffard,Stefanie R. Bailey,Praju V. Anekal,Paula D.L.M. Montero Llopis,Linda T. Nieman,Yuhui Song,Kedong Xu,Trisha R. Berger,Michael C. Kann,Mark B. Leick,Harrison Silva,Diego Salas‐Benito,Tamina Kienka,Korneel Grauwet,Todd D. Armstrong,Rui Zhang,Qingfeng Zhu,Juan Fu,Andrea Schmidts,Felix Korell,Max Jan,Bryan D. Choi,Andrew S. Liss,Genevieve M. Boland,David T. Ting,Richard A. Burkhart,Russell W. Jenkins,Zheng Li,Elizabeth M. Jaffee,Jacquelyn W. Zimmerman,Marcela V. Maus
出处
期刊:Clinical Cancer Research [American Association for Cancer Research]
卷期号:: OF1-OF19
标识
DOI:10.1158/1078-0432.ccr-23-3841
摘要

Abstract Purpose: Targeting solid tumors with chimeric antigen receptor (CAR) T cells remains challenging due to heterogenous target antigen expression, antigen escape, and the immunosuppressive tumor microenvironment (TME). Pancreatic cancer is characterized by a thick stroma generated by cancer-associated fibroblasts (CAF), which may contribute to the limited efficacy of mesothelin-directed CAR T cells in early-phase clinical trials. To provide a more favorable TME for CAR T cells to target pancreatic ductal adenocarcinoma (PDAC), we generated T cells with an antimesothelin CAR and a secreted T-cell–engaging molecule (TEAM) that targets CAF through fibroblast activation protein (FAP) and engages T cells through CD3 (termed mesoFAP CAR-TEAM cells). Experimental Design: Using a suite of in vitro, in vivo, and ex vivo patient-derived models containing cancer cells and CAF, we examined the ability of mesoFAP CAR-TEAM cells to target PDAC cells and CAF within the TME. We developed and used patient-derived ex vivo models, including patient-derived organoids with patient-matched CAF and patient-derived organotypic tumor spheroids. Results: We demonstrated specific and significant binding of the TEAM to its respective antigens (CD3 and FAP) when released from mesothelin-targeting CAR T cells, leading to T-cell activation and cytotoxicity of the target cell. MesoFAP CAR-TEAM cells were superior in eliminating PDAC and CAF compared with T cells engineered to target either antigen alone in our ex vivo patient-derived models and in mouse models of PDAC with primary or metastatic liver tumors. Conclusions: CAR-TEAM cells enable modification of tumor stroma, leading to increased elimination of PDAC tumors. This approach represents a promising treatment option for pancreatic cancer.
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