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猪内源性转座酶基因在人细胞和体内的过度激活。

Hyperactive piggyBac gene transfer in human cells and in vivo.

机构信息

Medical Scientist Training Program, Baylor College of Medicine, Houston, TX 77030, USA.

出版信息

Hum Gene Ther. 2012 Mar;23(3):311-20. doi: 10.1089/hum.2011.138. Epub 2011 Dec 14.

Abstract

We characterized a recently developed hyperactive piggyBac (pB) transposase enzyme [containing seven mutations (7pB)] for gene transfer in human cells in vitro and to somatic cells in mice in vivo. Despite a protein level expression similar to that of native pB, 7pB significantly increased the gene transfer efficiency of a neomycin resistance cassette transposon in both HEK293 and HeLa cultured human cells. Native pB and SB100X, the most active transposase of the Sleeping Beauty transposon system, exhibited similar transposition efficiency in cultured human cell lines. When delivered to primary human T cells ex vivo, 7pB increased gene delivery two- to threefold compared with piggyBac and SB100X. The activity of hyperactive 7pB transposase was not affected by the addition of a 24-kDa N-terminal tag, whereas SB100X manifested a 50% reduction in transposition. Hyperactive 7pB was compared with native pB and SB100X in vivo in mice using hydrodynamic tail-vein injection of a limiting dose of transposase DNA combined with luciferase reporter transposons. We followed transgene expression for up to 6 months and observed approximately 10-fold greater long-term gene expression in mice injected with a codon-optimized version of 7pB compared with mice injected with native pB or SB100X. We conclude that hyperactive piggyBac elements can increase gene transfer in human cells and in vivo and should enable improved gene delivery using the piggyBac transposon system in a variety of cell and gene-therapy applications.

摘要

我们对最近开发的一种活性增强型猪gyBac(pB)转座酶[含有七个突变(7pB)]进行了研究,该酶用于体外人细胞和体内小鼠体细胞中的基因转移。尽管其蛋白水平表达与天然 pB 相似,但 7pB 显著提高了新霉素抗性盒转座子在 HEK293 和 HeLa 培养的人细胞中的基因转移效率。天然 pB 和 SB100X(Sleeping Beauty 转座子系统中活性最强的转座酶)在培养的人细胞系中表现出相似的转座效率。当将其递送至体外原代人 T 细胞时,与 pB 和 SB100X 相比,7pB 将基因传递增加了两到三倍。活性增强的 7pB 转座酶的活性不受添加 24kDa N 端标签的影响,而 SB100X 的转座则减少了 50%。通过尾静脉注射限制剂量的转座酶 DNA 并结合荧光素酶报告转座子,在体内小鼠中比较了活性增强的 7pB 与天然 pB 和 SB100X。我们跟踪了转基因表达长达 6 个月,并观察到用密码子优化的 7pB 注射的小鼠中的长期基因表达增加了约 10 倍,而用天然 pB 或 SB100X 注射的小鼠则没有。我们得出结论,活性增强型猪gyBac 元件可以提高人细胞和体内的基因转移效率,并且应该能够通过猪gyBac 转座子系统在各种细胞和基因治疗应用中提高基因传递效率。

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