CD20靶向嵌合抗原受体T细胞治疗非霍奇金淋巴瘤的临床前疗效
Pre-clinical efficacy of CD20-targeted chimeric antigen receptor T cells for non-Hodgkin's lymphoma.
作者信息
Wen Hairuo, Lou Xiaoyan, Qu Zhe, Qin Chao, Jiang Hua, Yang Ying, Kang Liqing, Geng Xingchao, Yu Lei, Huang Ying
机构信息
Key Laboratory of Beijing for Safety Evaluation of Drugs, National Center for Safety Evaluation of Drugs, National Institutes for Food and Drug Control, Beijing, 100176, People's Republic of China.
Shanghai Unicar-Therapy Bio-Medicine Technology Co., Ltd, No 1525 Minqiang Road, Shanghai, People's Republic of China.
出版信息
Discov Oncol. 2022 Nov 9;13(1):122. doi: 10.1007/s12672-022-00588-w.
BACKGROUND
A 4-1BB/CD3-ζ-costimulated CAR-T against CD20 (CAR-T20) was subjected to a systemic efficacy evaluation in a cell co-culture model, and NOD-SCID IL-2 receptor gamma null mice (short for NSG mice) were xenografted with human Burkitt's lymphoma Raji cells.
METHODS
CAR-T20 cells were incubated with target cells (K562, K562 CD20 or Raji cells) at ratios of 10:1 and 5:1 for 24 h, and the killing rate was estimated by an LDH cytotoxicity assay. To evaluate the effect of CAR-T20 on the survival time of tumor-bearing animals, 30 NSG mice were employed, and Raji-Luc cells (5 × 10 cells per mouse) were administered prior to CAR-T20 administration. The survival time, optical intensity of Raji-Luc cells, clinical symptoms, and body mass of the animals were observed. Another 144 male NSG mice were employed to investigate the proliferation and antitumor effects of CAR-T20. Human cytokine and murine cytokines were detected at 1, 7, 14, 21, 28, 42, 56 and 90 days post-CAR-T administration, while biochemistry index analysis, T-cell and CAR-T-cell detection in peripheral blood, and histopathological examination were performed at 14, 28, 56 and 90 days post-administration.
RESULTS
CAR-T20 cells had a specific killing effect on CD20-expressing cells in vitro. At a dose of 1 × 10 per mouse or above, CAR-T20 prolonged the median survival time from 14 days to more than 3 months, inhibited the proliferation of Raji cells in mice, and alleviated the clinical manifestations and weight loss caused by the Raji-Luc cell load. CAR-T20 at a dose of 2 × 10 per mouse or above inhibited the proliferation of Raji cells in mice for up to 111 days post-administration without recurrence. The numbers of T cells and CAR-T cells in the animals administered CAR-T20 increased significantly when Raji cells were markedly proliferated and subsequently decreased when Raji cells were predominantly inhibited. CAR-T20 increased human IFN-γ, murine TNF and murine IL-6 levels and decreased human IL-10 levels in tumor-bearing mice. The incidences of xenografted tumors in organs/tissues were also reduced effectively by CAR-T20.
CONCLUSION
The effective dose of CAR-T20 in mice starts from 1 × 10 per mouse, equivalent to a clinical dose of 5 × 10/kg. Together, our data support the clinical translation of CAR-T20 for R/R B-cell NHL patients.
背景
在细胞共培养模型中对一种4-1BB/CD3-ζ共刺激的抗CD20嵌合抗原受体T细胞(CAR-T20)进行了全身疗效评估,并用人伯基特淋巴瘤Raji细胞对NOD-SCID白细胞介素2受体γ链缺陷小鼠(简称NSG小鼠)进行异种移植。
方法
将CAR-T20细胞与靶细胞(K562、K562 CD20或Raji细胞)按10:1和5:1的比例孵育24小时,并通过乳酸脱氢酶(LDH)细胞毒性试验评估杀伤率。为评估CAR-T20对荷瘤动物生存时间的影响,使用了30只NSG小鼠,在给予CAR-T20之前先注射Raji-Luc细胞(每只小鼠5×10个细胞)。观察动物的生存时间、Raji-Luc细胞的光强度、临床症状和体重。另外使用144只雄性NSG小鼠研究CAR-T20的增殖和抗肿瘤作用。在给予CAR-T后1、7、14、21、28、42、56和90天检测人细胞因子和鼠细胞因子,同时在给药后14、28、56和90天进行生化指标分析、外周血T细胞和CAR-T细胞检测以及组织病理学检查。
结果
CAR-T20细胞在体外对表达CD20的细胞具有特异性杀伤作用。每只小鼠剂量为1×10或更高时,CAR-T20将中位生存时间从14天延长至3个月以上,抑制了小鼠体内Raji细胞的增殖,并减轻了Raji-Luc细胞负荷引起的临床表现和体重减轻。每只小鼠剂量为2×10或更高时,CAR-T20在给药后长达111天抑制小鼠体内Raji细胞的增殖且无复发。给予CAR-T20的动物中,当Raji细胞明显增殖时T细胞和CAR-T细胞数量显著增加,而当Raji细胞主要被抑制时数量随后减少。CAR-T20增加了荷瘤小鼠体内人干扰素-γ、鼠肿瘤坏死因子和鼠白细胞介素-6水平,并降低了人白细胞介素-10水平。CAR-T20还有效降低了器官/组织中异种移植肿瘤的发生率。
结论
CAR-T20在小鼠中的有效剂量从每只小鼠1×10开始,相当于临床剂量5×10/kg。总之,我们的数据支持CAR-T20用于复发/难治性B细胞非霍奇金淋巴瘤(R/R B-cell NHL)患者的临床转化。
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