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血清补充细胞培养基中DNA链置换电路的设计与表征

Design and Characterization of DNA Strand-Displacement Circuits in Serum-Supplemented Cell Medium.

作者信息

Fern Joshua, Schulman Rebecca

机构信息

Chemical and Biomolecular Engineering, Johns Hopkins University , Baltimore, Maryland 21218, United States.

Computer Science, Johns Hopkins University , Baltimore, Maryland 21218, United States of America.

出版信息

ACS Synth Biol. 2017 Sep 15;6(9):1774-1783. doi: 10.1021/acssynbio.7b00105. Epub 2017 Jun 13.

Abstract

The functional stability and lifetimes of synthetic molecular circuits in biological environments are important for long-term, stable sensors or controllers of cell or tissue behavior. DNA-based molecular circuits, in particular DNA strand-displacement circuits, provide simple and effective biocompatible control mechanisms and sensors, but are vulnerable to digestion by nucleases present in living tissues and serum-supplemented cell culture. The stability of double-stranded and single-stranded DNA circuit components in serum-supplemented cell medium and the corresponding effect of nuclease-mediated degradation on circuit performance were characterized to determine the major routes of degradation and DNA strand-displacement circuit failure. Simple circuit design choices, such as the use of 5' toeholds within the DNA complexes used as reactants in the strand-displacement reactions and the termination of single-stranded components with DNA hairpin domains at the 3' termini, significantly increase the functional lifetime of the circuit components in the presence of nucleases. Simulations of multireaction circuits, guided by the experimentally measured operation of single-reaction circuits, enable predictive realization of multilayer and competitive-reaction circuit behavior. Together, these results provide a basic route to increased DNA circuit stability in cell culture environments.

摘要

合成分子电路在生物环境中的功能稳定性和寿命对于长期稳定地传感或控制细胞或组织行为至关重要。基于DNA的分子电路,特别是DNA链置换电路,提供了简单有效的生物相容性控制机制和传感器,但易被活组织和补充血清的细胞培养物中存在的核酸酶消化。对双链和单链DNA电路组件在补充血清的细胞培养基中的稳定性以及核酸酶介导的降解对电路性能的相应影响进行了表征,以确定主要的降解途径和DNA链置换电路故障。简单的电路设计选择,例如在链置换反应中用作反应物的DNA复合物中使用5' 起始端,以及在3' 末端用DNA发夹结构域终止单链组件,在存在核酸酶的情况下显著增加了电路组件的功能寿命。在单反应电路的实验测量操作指导下对多反应电路进行模拟,能够预测性地实现多层和竞争反应电路行为。这些结果共同提供了一条提高细胞培养环境中DNA电路稳定性的基本途径。

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