Zuo Yihan, Vohwinkel David J, Dong Bowen, McDowell James R, Guzman Brandon V, Manickavel Pandian Tharuna Sri, Chattopadhyay Saborni, McGray A J R, Olejniczak Scott H, Ohm Joyce, Wang Jianmin, Long Mark D, Gomez Eduardo Cortes, Purdon Terence J, Luo Wei, Mohammadpour Hemn, Hackett Christopher S, Cherkassky Leonid, Davila Marco, Abrams Scott I, Brentjens Renier J
Department of Medicine, Roswell Park Comprehensive Cancer Center, Buffalo, NY 14263, USA.
Department of Immunology, Roswell Park Comprehensive Cancer Center, Buffalo, NY 14263, USA.
Cancer Cell. 2026 Feb 9;44(2):366-382.e10. doi: 10.1016/j.ccell.2025.11.007. Epub 2025 Dec 11.
Chimeric antigen receptor (CAR) T cells are ineffective against solid tumors due to obstacles of antigen heterogeneity and the immunosuppressive tumor microenvironment (TME). Previous efforts focused on enhancing cytotoxicity and persistence of CAR T cells, while the feasibility of improving their therapeutic efficacy by leveraging the modulatory effects of CAR T cells on host anti-tumor immunity remains unclear. Here, we report that IL-36γ armored CAR T cells eradicate primary solid tumors and enable rejection of rechallenged antigen-negative tumors. IL-36γ armored CAR T cells favorably modulate the TME and reprogram unique neutrophil subsets with tumoricidal ability and antigen-(cross) presenting functions, resulting in the induction of endogenous T cells recognizing tumor antigens beyond CAR-targeted antigens. Our study demonstrates that neutrophil engagement by CAR T cells is a critical step in the establishment of the cancer-immunity cycle and introduces a broadly applicable method to overcome key barriers to adoptive cell therapies for solid tumors.
嵌合抗原受体(CAR)T细胞由于抗原异质性和免疫抑制性肿瘤微环境(TME)的障碍,对实体瘤无效。以往的研究主要集中在增强CAR T细胞的细胞毒性和持久性,而利用CAR T细胞对宿主抗肿瘤免疫的调节作用来提高其治疗效果的可行性仍不明确。在此,我们报告白细胞介素-36γ(IL-36γ)武装的CAR T细胞可根除原发性实体瘤,并能排斥再次攻击的抗原阴性肿瘤。IL-36γ武装的CAR T细胞可有利地调节TME,并重新编程具有杀瘤能力和抗原(交叉)呈递功能的独特中性粒细胞亚群,从而诱导内源性T细胞识别CAR靶向抗原以外的肿瘤抗原。我们的研究表明,CAR T细胞与中性粒细胞的相互作用是建立癌症免疫循环的关键步骤,并引入了一种广泛适用的方法来克服实体瘤过继性细胞治疗的关键障碍。
