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基于赛米利疱疹病毒的基因递送载体在体外小鼠胚胎干细胞分化过程中维持异源基因表达。

Herpesvirus saimiri-based gene delivery vectors maintain heterologous expression throughout mouse embryonic stem cell differentiation in vitro.

作者信息

Stevenson A J, Clarke D, Meredith D M, Kinsey S E, Whitehouse A, Bonifer C

机构信息

Molecular Medicine Unit, University of Leeds, St James's University Hospital, UK.

出版信息

Gene Ther. 2000 Mar;7(6):464-71. doi: 10.1038/sj.gt.3301130.

Abstract

In order to achieve a high efficiency of gene delivery into rare cell types like stem cells the use of viral vectors is presently without alternative. An ideal stem cell gene therapy vector would be able to infect primitive progenitor cells and sustain or activate gene expression in differentiated progeny. However, many viral vectors are inactivated when introduced in developing systems where cell differentiation occurs. To this end, we have developed a mouse in vitro model for testing herpesvirus saimiri (HVS)-based gene therapy vectors. We demonstrate here for the first time that HVS is able to infect totipotent mouse embryonic stem (ES) cells with high efficiency. We have transduced ES cells with a recombinant virus carrying the enhanced green fluorescent protein (EGFP) gene and the neomycin resistance gene (NeoR) driven by a CMV promoter and the SV40 promoter, respectively. ES cells maintain the viral episomal genome and can be terminally differentiated into mature haematopoietic cells. Moreover, heterologous gene expression is maintained throughout in vitro differentiation. Besides its obvious use in gene therapy, this unique expression system has wide ranging applications in studies aimed at understanding gene function and expression in cell differentiation and development.

摘要

为了实现将基因高效递送至干细胞等稀有细胞类型中,目前使用病毒载体是别无他法的选择。理想的干细胞基因治疗载体应能够感染原始祖细胞,并在分化后的子代细胞中维持或激活基因表达。然而,当许多病毒载体被引入发生细胞分化的发育系统中时,它们会失活。为此,我们开发了一种小鼠体外模型,用于测试基于猴疱疹病毒(HVS)的基因治疗载体。我们在此首次证明,HVS能够高效感染全能性小鼠胚胎干细胞(ES细胞)。我们用一种重组病毒转导ES细胞,该重组病毒分别携带由巨细胞病毒(CMV)启动子和猴空泡病毒40(SV40)启动子驱动的增强型绿色荧光蛋白(EGFP)基因和新霉素抗性基因(NeoR)。ES细胞维持病毒附加型基因组,并且可以终末分化为成熟的造血细胞。此外,在整个体外分化过程中,异源基因表达得以维持。除了在基因治疗中的明显用途外,这种独特的表达系统在旨在了解细胞分化和发育过程中基因功能和表达的研究中具有广泛的应用。

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