CD20
嵌合抗原受体
淋巴瘤
医学
T细胞
离体
抗原
癌症研究
体内
细胞疗法
临床试验
免疫学
细胞
病理
生物
免疫系统
遗传学
生物技术
作者
M. Kazim Panjwani,Matthew J. Atherton,Martha A. MaloneyHuss,Kumudhini Preethi Haran,Ailian Xiong,Minnal Gupta,Irina Kulikovsaya,Simon F. Lacey,Nicola J. Mason
出处
期刊:OncoImmunology
[Landes Bioscience]
日期:2019-10-23
卷期号:9 (1): 1676615-1676615
被引量:67
标识
DOI:10.1080/2162402x.2019.1676615
摘要
Multiple rodent and primate preclinical studies have advanced CAR T cells into the clinic. However, no single model accurately reflects the challenges of effective CAR T therapy in human cancer patients. To evaluate the effectiveness of next-generation CAR T cells that aim to overcome barriers to durable tumor elimination, we developed a system to evaluate CAR T cells in pet dogs with spontaneous cancer. Here we report on this system and the results of a pilot trial using CAR T cells to treat canine diffuse large B cell lymphoma (DLBCL). We designed and manufactured CD20-targeting, second-generation canine CAR T cells for functional evaluation in vitro and in vivo using lentivectors to parallel human CAR T cell manufacturing. A first-in-species trial of five dogs with DLBCL treated with CAR T was undertaken. Canine CAR T cells functioned in an antigen-specific manner and killed CD20+ targets. Circulating CAR T cells were detectable post-infusion, however, induction of canine anti-mouse antibodies (CAMA) was associated with CAR T cell loss. Specific selection pressure on CD20+ tumors was observed following CAR T cell therapy, culminating in antigen escape and emergence of CD20-disease. Patient survival times correlated with ex vivo product expansion. Altering product manufacturing improved transduction efficiency and skewed toward a memory-like phenotype of canine CAR T cells. Manufacturing of functional canine CAR T cells using a lentivector is feasible. Comparable challenges to effective CAR T cell therapy exist, indicating their relevance in informing future human clinical trial design.
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