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Synthetic switch-based baculovirus for transgene expression control and selective killing of hepatocellular carcinoma cells

机译:基于合成开关的杆状病毒用于转基因表达控制和选择性杀死肝癌细胞

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摘要

Baculovirus (BV) holds promise as a vector for anticancer gene delivery to combat the most common liver cancer–hepatocellular carcinoma (HCC). However, in vivo BV administration inevitably results in BV entry into non-HCC normal cells, leaky anticancer gene expression and possible toxicity. To improve the safety, we employed synthetic biology to engineer BV for transgene expression regulation. We first uncovered that miR-196a and miR-126 are exclusively expressed in HCC and normal cells, respectively, which allowed us to engineer a sensor based on distinct miRNA expression signature. We next assembled a synthetic switch by coupling the miRNA sensor and RNA binding protein L7Ae for translational repression, and incorporated the entire device into a single BV. The recombinant BV efficiently entered HCC and normal cells and enabled cis-acting transgene expression control, by turning OFF transgene expression in normal cells while switching ON transgene expression in HCC cells. Using pro-apoptotic hBax as the transgene, the switch-based BV selectively killed HCC cells in separate culture and mixed culture of HCC and normal cells. These data demonstrate the potential of synthetic switch-based BV to distinguish HCC and non-HCC normal cells for selective transgene expression control and killing of HCC cells.
机译:杆状病毒(BV)有望作为抗癌基因传递的载体,与最常见的肝癌-肝细胞癌(HCC)作斗争。但是,体内BV给药不可避免地导致BV进入非HCC正常细胞,抗癌基因表达漏失和可能的毒性。为了提高安全性,我们采用了合成生物学技术对BV进行转基因表达调控。我们首先发现miR-196a和miR-126分别在HCC和正常细胞中表达,这使我们能够设计基于不同miRNA表达特征的传感器。接下来,我们通过偶联miRNA传感器和RNA结合蛋白L7Ae进行翻译抑制,组装了一个合成开关,并将整个设备整合到一个BV中。重组BV通过关闭正常细胞中的转基因表达,同时打开HCC细胞中的转基因表达,有效地进入肝细胞和正常细胞,并实现顺式作用转基因表达控制。使用促凋亡的hBax作为转基因,基于开关的BV在HCC和正常细胞的单独培养和混合培养中选择性杀死HCC细胞。这些数据证明了基于合成开关的BV区分HCC和非HCC正常细胞进行选择性转基因表达控制和杀死HCC细胞的潜力。

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