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本文引用的文献

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Robust multicellular computing using genetically encoded NOR gates and chemical 'wires'.使用基因编码的 NOR 门和化学“导线”进行稳健的多细胞计算。
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Toward scalable parts families for predictable design of biological circuits.迈向可扩展的部件家族,以实现生物电路的可预测设计。
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多功能 RNA 感应转录调控因子用于工程遗传网络。

Versatile RNA-sensing transcriptional regulators for engineering genetic networks.

机构信息

Department of Bioengineering, University of California, Berkeley, CA 94720, USA.

出版信息

Proc Natl Acad Sci U S A. 2011 May 24;108(21):8617-22. doi: 10.1073/pnas.1015741108. Epub 2011 May 9.

DOI:10.1073/pnas.1015741108
PMID:21555549
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3102349/
Abstract

The widespread natural ability of RNA to sense small molecules and regulate genes has become an important tool for synthetic biology in applications as diverse as environmental sensing and metabolic engineering. Previous work in RNA synthetic biology has engineered RNA mechanisms that independently regulate multiple targets and integrate regulatory signals. However, intracellular regulatory networks built with these systems have required proteins to propagate regulatory signals. In this work, we remove this requirement and expand the RNA synthetic biology toolkit by engineering three unique features of the plasmid pT181 antisense-RNA-mediated transcription attenuation mechanism. First, because the antisense RNA mechanism relies on RNA-RNA interactions, we show how the specificity of the natural system can be engineered to create variants that independently regulate multiple targets in the same cell. Second, because the pT181 mechanism controls transcription, we show how independently acting variants can be configured in tandem to integrate regulatory signals and perform genetic logic. Finally, because both the input and output of the attenuator is RNA, we show how these variants can be configured to directly propagate RNA regulatory signals by constructing an RNA-meditated transcriptional cascade. The combination of these three features within a single RNA-based regulatory mechanism has the potential to simplify the design and construction of genetic networks by directly propagating signals as RNA molecules.

摘要

RNA 广泛感知小分子和调节基因的天然能力已成为合成生物学的重要工具,其应用范围广泛,包括环境感应和代谢工程。在 RNA 合成生物学的先前工作中,已经设计了独立调节多个靶标的 RNA 机制,并整合了调节信号。然而,使用这些系统构建的细胞内调控网络需要蛋白质来传播调控信号。在这项工作中,我们通过设计质粒 pT181 反义 RNA 介导的转录衰减机制的三个独特特性,消除了这一要求并扩展了 RNA 合成生物学工具包。首先,由于反义 RNA 机制依赖于 RNA-RNA 相互作用,我们展示了如何对天然系统的特异性进行工程设计,以创建能够在同一细胞中独立调节多个靶标的变体。其次,由于 pT181 机制控制转录,我们展示了如何将独立作用的变体串联配置,以整合调节信号并执行遗传逻辑。最后,由于衰减器的输入和输出都是 RNA,我们展示了如何通过构建 RNA 介导的转录级联来配置这些变体,以直接传播 RNA 调节信号。在单个基于 RNA 的调控机制中组合这三个特性,有可能通过将信号直接作为 RNA 分子进行传播,从而简化遗传网络的设计和构建。