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通过工程化锌指 DNA 结合域重新定位睡眠美人转座子插入。

Retargeting sleeping beauty transposon insertions by engineered zinc finger DNA-binding domains.

机构信息

Max Delbrück Center for Molecular Medicine, Berlin, Germany.

出版信息

Mol Ther. 2012 Oct;20(10):1852-62. doi: 10.1038/mt.2012.126. Epub 2012 Jul 10.

Abstract

The Sleeping Beauty (SB) transposon is a nonviral, integrating vector system with proven efficacy in preclinical animal models, and thus holds promise for future clinical applications. However, SB has a close-to-random insertion profile that could lead to genotoxic effects, thereby presenting a potential safety issue. We evaluated zinc finger (ZF) DNA-binding domains (DBDs) for their abilities to introduce a bias into SB's insertion profile. E2C, that binds a unique site in the erbB-2 gene, mediated locus-specific transposon insertions at low frequencies. A novel ZF targeting LINE1 repeats, ZF-B, showed specific binding to an 18-bp site represented by ~12,000 copies in the human genome. We mapped SB insertions using linear-amplification (LAM)-PCR and Illumina sequencing. Targeted insertions with ZF-B peaked at approximately fourfold enrichment of transposition around ZF-B binding sites yielding ~45% overall frequency of insertion into LINE1. A decrease in the ZF-B dataset with respect to transposon insertions in genes was found, suggesting that LINE1 repeats act as a sponge that "soak up" a fraction of SB insertions and thereby redirect them away from genes. Improvements in ZF technology and a careful choice of targeted genomic regions may improve the safety profile of SB for future clinical applications.

摘要

睡眠美人(SB)转座子是一种非病毒整合载体系统,在临床前动物模型中已被证明具有疗效,因此有望在未来的临床应用中得到应用。然而,SB 的插入谱接近随机,可能导致遗传毒性效应,从而带来潜在的安全问题。我们评估了锌指(ZF)DNA 结合域(DBD)将 SB 的插入谱引入偏向的能力。E2C 结合 erbB-2 基因中的独特位点,以低频率介导基因座特异性转座子插入。一种针对 LINE1 重复序列的新型 ZF,ZF-B,表现出对人类基因组中约 12000 个拷贝代表的 18 个碱基对位点的特异性结合。我们使用线性扩增(LAM)-PCR 和 Illumina 测序来绘制 SB 插入图谱。ZF-B 的靶向插入在 ZF-B 结合位点周围的转位富集峰值约为四,总体插入 LINE1 的频率约为 45%。在基因中转座子插入方面,ZF-B 数据集减少,这表明 LINE1 重复序列充当“海绵”,吸收了 SB 插入的一部分,并将其重新引导远离基因。改进 ZF 技术和谨慎选择靶向基因组区域可能会提高 SB 未来临床应用的安全性。

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