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基于变构调节的触发点介导链位移电路的合理设计用于小分子代谢物的灵敏和现场检测。

Rational design of allosterically regulated toehold mediated strand displacement circuits for sensitive and on-site detection of small molecule metabolites.

机构信息

Department of Chemical and Biological Engineering, The Hong Kong University of Science and Technology, Clear Water Bay, Kowloon, Hong Kong, China.

出版信息

Analyst. 2021 Nov 22;146(23):7144-7151. doi: 10.1039/d1an01488a.

DOI:10.1039/d1an01488a
PMID:34734587
Abstract

Development of small molecule biosensors enables rapid and de-centralized small molecule detection that meets the demands of routine health monitoring and rapid diagnosis. Among them, allosteric transcription factor (aTF)-based biosensors have shown potential in modular design of small molecule detection platforms due to their ligand-regulated DNA binding activity. Here, we expand the capabilities of a biosensor that leverages the aTF-based regulation of toehold-mediated strand displacement (TMSD) circuits for uric acid (UA) detection in non-invasive salivary samples by utilizing the UA-responsive aTF HucR. The impact of the low ligand affinity of the native HucR was addressed by engineering a two-pass TMSD circuit with rational design. This combined strategy achieved enrichment of the output signal and overcame the negative impact of the matrix effect on the sensitivity and overall response of the biosensor when using real samples, which enabled semi-quantitative detection in the normal salivary UA levels. As well, enhancements provided by the two-pass design halved the turnaround time to less than 15 minutes. To sum up, the two-cycle DNA circuit design enabled aTF-based simple, rapid and one-step non-invasive salivary UA detection, showing its potential in metabolite detection for health monitoring.

摘要

小分子生物传感器的发展使得快速和去中心化的小分子检测成为可能,满足了常规健康监测和快速诊断的需求。其中,变构转录因子(aTF)为基础的生物传感器由于其配体调节的 DNA 结合活性,在小分子检测平台的模块化设计中显示出了潜力。在这里,我们扩展了一种生物传感器的功能,该传感器利用基于 aTF 的调控,实现了对非侵入性唾液样本中尿酸(UA)的检测,该传感器利用了UA 响应型 aTF HucR。通过合理设计,构建了双通路的 TMSD 电路,解决了天然 HucR 配体亲和力低的问题。该组合策略实现了输出信号的富集,并克服了使用实际样本时基质效应对生物传感器的灵敏度和整体响应的负面影响,从而能够对半定量检测正常唾液中的 UA 水平。此外,双通路设计将检测时间缩短至 15 分钟以内。总之,双循环 DNA 电路设计使得基于 aTF 的简单、快速和一步非侵入性唾液 UA 检测成为可能,为健康监测中的代谢物检测展示了其潜力。

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