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四环素阻遏蛋白tetR而非tetR-哺乳动物细胞转录因子融合衍生物调控哺乳动物细胞中的诱导型基因表达。

Tetracycline repressor, tetR, rather than the tetR-mammalian cell transcription factor fusion derivatives, regulates inducible gene expression in mammalian cells.

作者信息

Yao F, Svensjö T, Winkler T, Lu M, Eriksson C, Eriksson E

机构信息

Division of Plastic Surgery, Brigham and Women's Hospital, Boston, MA 02115, USA.

出版信息

Hum Gene Ther. 1998 Sep 1;9(13):1939-50. doi: 10.1089/hum.1998.9.13-1939.

Abstract

This article describes the first (to our knowledge) tetracycline-inducible regulatory system that demonstrates that the tetracycline repressor (tetR) alone, rather than tetR-mammalian cell transcription factor fusion derivatives, can function as a potent trans-modulator to regulate gene expression in mammalian cells. With proper positioning of tetracycline operators downstream of the TATA element and of human epidermal growth factor (hEGF) as a reporter, we show that gene expression from the tetracycline operator-bearing hCMV major immediate-early enhancer-promoter (pcmvtetO) can be regulated by tetR over three orders of magnitude in response to tetracycline when (1) the reporter was cotransfected with tetR-expressing plasmid in transient expression assays, and (2) the reporter unit was stably integrated into the chromosome of a tetR-expressing cell line. This level of tetR-mediated inducible gene regulation is significantly higher than that of other repression-based mammalian cell transcription switch systems. In an in vivo porcine wound model, close to 60-fold tetR-mediated regulatory effects were detected and it was reversed when tetracycline was administered. Collectively, this study provides a direct implementation of this tetracycline-inducible regulatory switch for controlling gene expression in vitro, in vivo, and in gene therapy.

摘要

本文描述了首个(据我们所知)四环素诱导调控系统,该系统表明单独的四环素阻遏物(tetR),而非tetR-哺乳动物细胞转录因子融合衍生物,可作为一种有效的反式调节因子来调控哺乳动物细胞中的基因表达。通过将四环素操纵子正确定位在TATA元件下游,并以人表皮生长因子(hEGF)作为报告基因,我们发现当(1)在瞬时表达实验中将报告基因与表达tetR的质粒共转染,以及(2)将报告基因单元稳定整合到表达tetR的细胞系染色体中时,携带四环素操纵子的人巨细胞病毒主要立即早期增强子-启动子(pcmvtetO)的基因表达可因四环素而在三个数量级范围内受到tetR的调控。tetR介导的这种诱导型基因调控水平显著高于其他基于阻遏的哺乳动物细胞转录开关系统。在体内猪伤口模型中,检测到了近60倍的tetR介导的调控效应,并且在给予四环素后该效应逆转。总体而言,本研究为这种四环素诱导调控开关在体外、体内及基因治疗中控制基因表达提供了直接的应用。

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