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Engineering protein-protein devices for multilayered regulation of mRNA translation using orthogonal proteases in mammalian cells

机译:工程蛋白-蛋白设备用于在哺乳动物细胞中使用正交蛋白酶对mRNA翻译进行多层调节

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摘要

The development of RNA-encoded regulatory circuits relying on RNA-binding proteins (RBPs) has enhanced the applicability and prospects of post-transcriptional synthetic network for reprogramming cellular functions. However, the construction of RNA-encoded multilayer networks is still limited by the availability of composable and orthogonal regulatory devices. Here, we report on control of mRNA translation with newly engineered RBPs regulated by viral proteases in mammalian cells. By combining post-transcriptional and post-translational control, we expand the operational landscape of RNA-encoded genetic circuits with a set of regulatory devices including: i) RBP-protease, ii) protease-RBP, iii) protease–protease, iv) protein sensor protease-RBP, and v) miRNA-protease/RBP interactions. The rational design of protease-regulated proteins provides a diverse toolbox for synthetic circuit regulation that enhances multi-input information processing-actuation of cellular responses. Our approach enables design of artificial circuits that can reprogram cellular function with potential benefits as research tools and for future in vivo therapeutics and biotechnological applications.
机译:依赖RNA结合蛋白(RBPs)的RNA编码调控电路的发展增强了转录后合成网络对细胞功能进行重新编程的适用性和前景。但是,RNA编码多层网络的构建仍然受到可组合和正交调节装置的可用性的限制。在这里,我们报道了哺乳动物细胞中病毒蛋白酶调节的新设计的RBPs对mRNA翻译的控制。通过结合转录后和翻译后控制,我们通过一套调控装置扩展了RNA编码的遗传回路的操作范围,这些调控装置包括:i)RBP蛋白酶,ii)蛋白酶-RBP,iii)蛋白酶-蛋白酶,iv)蛋白传感器蛋白酶-RBP,以​​及v)miRNA-蛋白酶/ RBP相互作用。蛋白酶调节蛋白的合理设计为合成电路调节提供了多样化的工具箱,从而增强了细胞反应的多输入信息处理的启动。我们的方法可以设计人造电路,从而可以重新编程细胞功能,并具有潜在的优势,可以作为研究工具并用于未来的体内治疗和生物技术应用。

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