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利用 piggyBac 转座子/转座酶系统生成针对 CD19 的 T 细胞用于治疗 B 细胞恶性肿瘤。

piggyBac transposon/transposase system to generate CD19-specific T cells for the treatment of B-lineage malignancies.

机构信息

Division of Pediatrics, University of Texas MD Anderson Cancer Center, Houston, TX 77030, USA.

出版信息

Hum Gene Ther. 2010 Apr;21(4):427-37. doi: 10.1089/hum.2009.114.

Abstract

Nonviral integrating vectors can be used for expression of therapeutic genes. piggyBac (PB), a transposon/transposase system, has been used to efficiently generate induced pluripotent stems cells from somatic cells, without genetic alteration. In this paper, we apply PB transposition to express a chimeric antigen receptor (CAR) in primary human T cells. We demonstrate that T cells electroporated to introduce the PB transposon and transposase stably express CD19-specific CAR and when cultured on CD19(+) artificial antigen-presenting cells, numerically expand in a CAR-dependent manner, display a phenotype associated with both memory and effector T cell populations, and exhibit CD19-dependent killing of tumor targets. Integration of the PB transposon expressing CAR was not associated with genotoxicity, based on chromosome analysis. PB transposition for generating human T cells with redirected specificity to a desired target such as CD19 is a new genetic approach with therapeutic implications.

摘要

非病毒整合载体可用于治疗基因的表达。piggyBac(PB),一种转座子/转座酶系统,已被用于从体细胞中高效产生诱导多能干细胞,而不会引起遗传改变。在本文中,我们应用 PB 转座将嵌合抗原受体(CAR)表达在原代人 T 细胞中。我们证明,用电穿孔将 PB 转座子和转座酶引入的 T 细胞稳定表达 CD19 特异性 CAR,并且当在 CD19(+)人工抗原呈递细胞上培养时,以 CAR 依赖性方式在数量上扩增,表现出与记忆和效应 T 细胞群体相关的表型,并表现出对肿瘤靶标的 CD19 依赖性杀伤。基于染色体分析,表达 CAR 的 PB 转座子的整合与遗传毒性无关。PB 转座用于生成对目标如 CD19 具有重定向特异性的人 T 细胞是一种具有治疗意义的新的遗传方法。

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