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Self-adjusting synthetic gene circuit for correcting insulin resistance

机译:用于调节胰岛素抵抗的自调节合成基因电路

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摘要

By using tools from synthetic biology, sophisticated genetic devices can be assembled to reprogram mammalian cell activities. Here, we demonstrate that a self-adjusting synthetic gene circuit can be designed to sense and reverse the insulin-resistance syndrome in different mouse models. By functionally rewiring the mitogen-activated protein kinase (MAPK) signalling pathway to produce MAPK-mediated activation of the hybrid transcription factor TetR-ELK1, we assembled a synthetic insulin-sensitive transcription-control device that self-sufficiently distinguished between physiological and increased blood insulin levels and correspondingly fine-tuned the reversible expression of therapeutic transgenes from synthetic TetR-ELK1-specific promoters. In acute experimental hyperinsulinemia, the synthetic insulin-sensing designer circuit reversed the insulin-resistance syndrome by coordinating expression of the insulin-sensitizing compound adiponectin. Engineering synthetic gene circuits to sense pathologic markers and coordinate the expression of therapeutic transgenes may provide opportunities for future gene- and cell-based treatments of multifactorial metabolic disorders.
机译:通过使用来自合成生物学的工具,可以组装复杂的遗传设备以重新编程哺乳动物的细胞活动。在这里,我们证明了可以设计一种自我调节的合成基因电路,以感测和逆转不同小鼠模型中的胰岛素抵抗综合征。通过功能上重新连接丝裂原激活的蛋白激酶(MAPK)信号通路以产生MAPK介导的杂合转录因子TetR-ELK1的激活,我们组装了一种合成胰岛素敏感的转录控制设备,该设备可以自给自足地区分生理性血液和增加的血液胰岛素水平,并相应地微调了合成TetR-ELK1特异性启动子治疗性转基因的可逆表达。在急性实验性高胰岛素血症中,合成的胰岛素感应设计器电路通过协调胰岛素敏感性化合物脂联素的表达来逆转胰岛素抵抗综合征。工程化合成基因电路以感测病理标记并协调治疗性转基因的表达可能为未来基于基因和细胞的多因素代谢紊乱治疗提供机会。

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