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Boosting functionality of synthetic DNA circuits with tailored deactivation

机译:通过定制的失活增强合成DNA电路的功能

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摘要

Molecular programming takes advantage of synthetic nucleic acid biochemistry to assemble networks of reactions, in vitro, with the double goal of better understanding cellular regulation and providing information-processing capabilities to man-made chemical systems. The function of molecular circuits is deeply related to their topological structure, but dynamical features (rate laws) also play a critical role. Here we introduce a mechanism to tune the nonlinearities associated with individual nodes of a synthetic network. This mechanism is based on programming deactivation laws using dedicated saturable pathways. We demonstrate this approach through the conversion of a single-node homoeostatic network into a bistable and reversible switch. Furthermore, we prove its generality by adding new functions to the library of reported man-made molecular devices: a system with three addressable bits of memory, and the first DNA-encoded excitable circuit. Specific saturable deactivation pathways thus greatly enrich the functional capability of a given circuit topology.
机译:分子程序设计利用合成核酸生物化学技术在体外组装反应网络,双重目的是更好地了解细胞调节并为人造化学系统提供信息处理能力。分子电路的功能与其拓扑结构密切相关,但是动力学特征(速率定律)也起着至关重要的作用。在这里,我们介绍一种机制来调整与合成网络的各个节点相关的非线性。该机制基于使用专用的可饱和路径的编程去激活定律。我们通过将单节点同质网络转换为双稳态和可逆开关来演示这种方法。此外,我们通过向报告的人造分子设备库中添加新功能来证明其通用性:具有三个可寻址位的存储器系统以及第一个DNA编码的可激励电路。因此,特定的饱和失活路径极大地丰富了给定电路拓扑的功能。

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