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Stable gene transfer and expression in human primary T cells by the Sleeping Beauty transposon system

机译:睡美人转座子系统在人原代T细胞中稳定的基因转移和表达

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摘要

The Sleeping Beauty (SB) transposon system is a nonviral DNA delivery system in which a transposase directs integration of an SB transposon into TA-dinucleotide sites in the genome. To determine whether the SB transposon system can mediate stable gene expression in human T cells, primary peripheral blood lymphocytes (PBLs) were nucleofected with SB vectors carrying a DsRed reporter gene. Plasmids containing the SB transposase on the same molecule as (cis) or on a molecule separate from (trans) the SB transposon mediated long-term and stable reporter gene expression in human primary T cells. Sequencing of transposon:chromosome junctions confirmed that stable gene expression was due to SB-mediated transposition. In other studies, PBLs were successfully transfected using the SB transposon system and shown to stably express a fusion protein consisting of (1) a surface receptor useful for positive T-cell selection and (2) a “suicide” gene useful for elimination of transfected T cells after chemotherapy. This study is the first report demonstrating that the SB transposon system can mediate stable gene transfer in human primary PBLs, which may be advantageous for T-cell–based gene therapies.
机译:睡美人(SB)转座子系统是一种非病毒DNA传递系统,其中转座酶将SB转座子整合到基因组中的TA-二核苷酸位点。为了确定SB转座子系统是否可以介导人T细胞中稳定的基因表达,用携带DsRed报告基因的SB载体对原代外周血淋巴细胞(PBL)进行了核转染。在与顺式转座子相同的分子上或在与顺式转座子相同的分子上或与反式转座子分开的分子上含有SB转座酶的质粒,在人原代T细胞中介导了长期稳定的报告基因表达。转座子:染色体连接的测序证实稳定的基因表达归因于SB介导的转座。在其他研究中,使用SB转座子系统成功转染了PBL,并显示稳定表达融合蛋白,该融合蛋白由(1)用于阳性T细胞选择的表面受体和(2)用于消除转染的“自杀”基因组成化疗后的T细胞。这项研究是第一份证明SB转座子系统可以介导人类原发性PBLs中稳定基因转移的报告,这可能对基于T细胞的基因治疗有利。

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