Zheng Ai-Hong, Yu Chong, Su Yong-Rui, Peng Min, Chen Jian-Yuan, Wang Fu-Wei, Zhu Xiu-Ming, Yan Pei-Yuan, Wang Hai-Tao, Shen Jian, Chen Wei-Jun, Li Qiang, Chen Yuan, Chen Yi, Wang Yin-Shuang, Gu Hang-Yu, Meng Zhuo-Nan, Zhao Jing-Wen, Ni Wan-Mao, Wang Tian-Hua, Wu Sheng-Lian, Li Min, Wang Zheng, Cheng Ai-Ping, Huang Xiao-Xian, Yang Zi-Yan, Jiang Jia-Hong, Wang Qun-Jiang, Qu Jing, Zhang Shi-Tai, Shi Ke-Ke, Zhang Hua-Xin, Zhang Da-Hong, Wu Guo-Qing
Cancer Center, Department of Medical Oncology, Zhejiang Provincial People's Hospital, Affiliated People's Hospital, Hangzhou Medical College, Hangzhou, China.
Urology & Nephrology Center, Department of Urology, Zhejiang Provincial People's Hospital, Affiliated People's Hospital, Hangzhou Medical College, Hangzhou, China.
Transl Lung Cancer Res. 2025 Jul 31;14(7):2880-2890. doi: 10.21037/tlcr-2025-274. Epub 2025 Jul 28.
Cancer patients relapsing with leptomeningeal metastases (LM) but without extracranial lesions are usually unsuitable for cellular immunotherapy with tumor-infiltrating lymphocytes (TILs) owing to lack of tumor tissue. TILs generated from heavily pretreated patients, especially those with non-melanoma cancer often have anergic effects and are less toxic to tumors, limiting the antitumor efficacy of lymphocyte-based therapy. Whether using autologous tumor tissue banked in advance addresses the dilemma has not been explored.
We present two cases of non-small cell lung cancer (NSCLC) who relapsed with LM but without extracranial lesions for whom TIL therapy is otherwise unsuitable. Using autologous tumor tissue banked in advance when they initially underwent tumor resection, we successfully generated therapeutic TILs of which the enhancer of zeste homolog 2 (EZH2) activity was further inhibited in regulatory T cells (Tregs). One case received autologous TILs prepared from a cryopreserved pathological complete response lesion and achieved a complete remission of LM that was ongoing till the preparation of this manuscript. The other case was treated with autologous TILs derived from a cryopreserved treatment-naïve tumor tissue and only achieved a transient response manifested by short-term decrease of circulating tumor deoxyribonucleic acid and serum carcinoembryonic antigen.
TILs generated from treatment-responsive lesions and underwent inhibition of EZH2 activity in Tregs have high antitumor efficacy and the banking in advance of treatment-responsive tumor tissue potentially provides a safe and effective adoptive cell therapy (ACT) with TILs for refractory NSCLC patients with LM for whom TIL therapy is otherwise unsuitable.
癌症患者出现软脑膜转移(LM)但无颅外病变时,由于缺乏肿瘤组织,通常不适合采用肿瘤浸润淋巴细胞(TILs)进行细胞免疫治疗。从经过大量预处理的患者,尤其是非黑色素瘤癌症患者中产生的TILs往往具有无反应效应,对肿瘤的毒性较小,限制了基于淋巴细胞疗法的抗肿瘤疗效。预先储存自体肿瘤组织是否能解决这一困境尚未得到探索。
我们报告了两例非小细胞肺癌(NSCLC)患者,他们出现LM复发但无颅外病变,否则不适合进行TIL治疗。利用他们最初进行肿瘤切除时预先储存的自体肿瘤组织,我们成功产生了治疗性TILs,其中在调节性T细胞(Tregs)中zeste同源物2(EZH2)的活性进一步受到抑制。一例患者接受了从冷冻保存的病理完全缓解病变制备的自体TILs治疗,LM实现了完全缓解,直至撰写本稿件时仍在持续缓解。另一例患者接受了从冷冻保存的未经治疗的肿瘤组织衍生的自体TILs治疗,仅获得了短暂反应,表现为循环肿瘤脱氧核糖核酸和血清癌胚抗原短期下降。
从治疗反应性病变产生并在Tregs中EZH2活性受到抑制的TILs具有高抗肿瘤疗效,预先储存治疗反应性肿瘤组织可能为LM难治性NSCLC患者提供一种安全有效的TILs过继性细胞治疗(ACT),否则这些患者不适合进行TIL治疗。
