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De novo automated design of small RNA circuits for engineering synthetic riboregulation in living cells

机译:从头设计小RNA回路的自动化设计用于工程化活细胞中的合成核糖调节

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摘要

A grand challenge in synthetic biology is to use our current knowledge of RNA science to perform the automatic engineering of completely synthetic sequences encoding functional RNAs in living cells. We report here a fully automated design methodology and experimental validation of synthetic RNA interaction circuits working in a cellular environment. The computational algorithm, based on a physicochemical model, produces novel RNA sequences by exploring the space of possible sequences compatible with predefined structures. We tested our methodology in Escherichia coli by designing several positive riboregulators with diverse structures and interaction models, suggesting that only the energy of formation and the activation energy (free energy barrier to overcome for initiating the hybridization reaction) are sufficient criteria to engineer RNA interaction and regulation in bacteria. The designed sequences exhibit nonsignificant similarity to any known noncoding RNA sequence. Our riboregulatory devices work independently and in combination with transcription regulation to create complex logic circuits. Our results demonstrate that a computational methodology based on first-principles can be used to engineer interacting RNAs with allosteric behavior in living cells.
机译:合成生物学的一大挑战是利用我们目前对RNA科学的知识,对活细胞中编码功能性RNA的完全合成序列进行自动工程设计。我们在这里报告了在细胞环境中工作的合成RNA相互作用电路的全自动设计方法和实验验证。该计算算法基于物理化学模型,通过探索与预定结构兼容的可能序列的空间来产生新的RNA序列。我们通过设计具有不同结构和相互作用模型的几种阳性核糖调节剂,在大肠杆菌中测试了我们的方法,表明只有形成能和激活能(为克服杂交反应而克服的自由能垒)才是设计RNA相互作用和反应的足够标准。调节细菌。所设计的序列与任何已知的非编码RNA序列均显示出无显着相似性。我们的核糖调节仪可独立工作,并与转录调控结合使用,以创建复杂的逻辑电路。我们的结果表明,基于第一性原理的计算方法可用于工程设计相互作用的RNA与活细胞中的变构行为。

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