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Transcriptionally regulated and nontoxic delivery of the hyperactive Sleeping Beauty Transposase

机译:转录调节和无毒的过度活跃睡眠美容转座酶的交付。

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摘要

The Sleeping Beauty (SB) transposase and, in particular, its hyperactive variant SB100X raises increasing interest for gene therapy application, including genome modification and, more recently, induced pluripotent stem cells (iPS) reprogramming. The documented cytotoxicity of the transposase, when constitutively expressed by an integrating retroviral vector (iRV), has been circumvented by the transient delivery of SB100X using retroviral mRNA transfer. In this study, we developed an alternative, safe, and efficient transposase delivery system based on a tetracycline-ON regulated expression cassette and the rtTA2S-M2 transactivator gene transiently delivered by integration-defective lentiviral vectors (IDLVs). Compared with iRV-mediated delivery, expression of tetracycline-induced SB100X delivered by an IDLV results in more efficient integration of a GFP transposon and reduced toxicity. Tightly regulated expression and reactivation of the transposase was achieved in HeLa cells as wells as in human primary keratinocytes. Based on these properties, the regulated transposase-IDLV vectors may represent a valuable tool for genetic engineering and therapeutic gene transfer.
机译:睡美人(SB)转座酶,尤其是其过度活跃的变体SB100X,引起了人们对基因治疗应用的日益增长的兴趣,包括基因组修饰和最近诱导的多能干细胞(iPS)重编程。当转位酶由整合的逆转录病毒载体(iRV)组成型表达时,转座酶的细胞毒性已通过使用逆转录病毒mRNA转移瞬时递送SB100X来规避。在这项研究中,我们开发了一种基于四环素-ON调控表达盒和整合缺陷型慢病毒载体(IDLVs)瞬时递送的rtTA2 S -M2反激活基因的替代,安全,高效的转座酶递送系统)。与iRV介导的传递相比,IDLV传递的四环素诱导的SB100X的表达可更有效地整合GFP转座子并降低毒性。在HeLa细胞以及人类原代角质形成细胞中都实现了转座酶的严格调控表达和重新激活。基于这些性质,调控的转座酶-IDLV载体可以代表用于基因工程和治疗性基因转移的有价值的工具。

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