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Synthetic dual-input mammalian genetic circuits enable tunable and stringent transcription control by chemical and light

机译:合成双输入哺乳动物遗传电路可通过化学和光调节和严格控制转录

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摘要

Programmable transcription factors can enable precise control of gene expression triggered by a chemical inducer or light. To obtain versatile transgene system with combined benefits of a chemical inducer and light inducer, we created various chimeric promoters through the assembly of different copies of the tet operator and Gal4 operator module, which simultaneously responded to a tetracycline-responsive transcription factor and a light-switchable transactivator. The activities of these chimeric promoters can be regulated by tetracycline and blue light synergistically or antagonistically. Further studies of the antagonistic genetic circuit exhibited high spatiotemporal resolution and extremely low leaky expression, which therefore could be used to spatially and stringently control the expression of highly toxic protein Diphtheria toxin A for light regulated gene therapy. When transferring plasmids engineered for the gene switch-driven expression of a firefly luciferase (Fluc) into mice, the Fluc expression levels of the treated animals directly correlated with the tetracycline and light input program. We suggest that dual-input genetic circuits using TET and light that serve as triggers to achieve expression profiles may enable the design of robust therapeutic gene circuits for gene- and cell-based therapies.
机译:可编程转录因子可以精确控制由化学诱导物或光触发的基因表达。为了获得具有化学诱导剂和光诱导剂双重优势的通用转基因系统,我们通过组装不同拷贝的tet操纵子和Gal4操纵子模块创建了各种嵌合启动子,它们同时响应四环素响应转录因子和光可切换的反式激活剂。这些嵌合启动子的活性可以由四环素和蓝光协同或拮抗地调节。对拮抗性遗传回路的进一步研究显示出高的时空分辨率和极低的渗漏表达,因此可用于空间和严格控制高毒性蛋白白喉毒素A的表达,以用于调光基因治疗。当将工程改造为萤火虫荧光素酶(Fluc)的基因开关驱动表达的质粒转移到小鼠体内时,处理过的动物的Fluc表达水平与四环素和光输入程序直接相关。我们建议,使用TET和光作为实现表达谱的触发因素的双输入遗传电路可能使针对基因和细胞疗法的稳健治疗基因电路设计成为可能。

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