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无酶自动催化驱动反馈 DNA 电路用于活细胞的放大适体传感。

Enzyme-Free Autocatalysis-Driven Feedback DNA Circuits for Amplified Aptasensing of Living Cells.

机构信息

College of Chemistry and Molecular Sciences, Wuhan University, Wuhan 430072, P. R. China.

出版信息

ACS Appl Mater Interfaces. 2022 Feb 2;14(4):5080-5089. doi: 10.1021/acsami.1c22767. Epub 2022 Jan 19.

DOI:10.1021/acsami.1c22767
PMID:35044153
Abstract

Aptasensors with high specificity have emerged as powerful tools for understanding various biological processes, thus providing tremendous opportunities for clinical diagnosis and prognosis. However, their applications in intracellular molecular imaging are largely impeded due to the low anti-interference capacity in biological environments and the moderate sensitivity to targets. Herein, a robust enzyme-free autocatalysis-driven feedback DNA circuit is devised for amplified aptasensing, for example, adenosine triphosphate (ATP) and thrombin, with a significantly improved sensitivity in living cells. This initiator-replicated hybridization chain reaction (ID-HCR) circuit was acquired by integrating the HCR circuit with the DNAzyme biocatalysis. Also, the autocatalysis-driven aptasensor consists of a recognition element and an amplification element. The recognition unit can specifically identify ATP or thrombin via a versatile conformational transformation, resulting in the exposure of the initiator to the autocatalysis-driven circuit. The ID-HCR element integrates the charming self-assembly characteristics of the HCR and the remarkable catalytic cleavage capacity of DNAzyme for realizing the continuously self-sustained regeneration or replication of trigger strands and for achieving an exponential signal gain. The autocatalysis-driven aptasensor has been validated for quantitative analysis of ATP and thrombin in vitro and for monitoring the corresponding aptamer substrates with various expressions in live cells. More importantly, the autocatalysis-driven aptasensor, as a versatile amplification strategy, holds enormous potential for analysis of other less abundant biomarkers by changing only the recognition element of the system.

摘要

具有高特异性的适体传感器已成为理解各种生物过程的强大工具,从而为临床诊断和预后提供了巨大的机会。然而,由于在生物环境中低的抗干扰能力和对靶标适中的灵敏度,它们在细胞内分子成像中的应用受到了很大的限制。在此,设计了一种稳健的无酶自动催化驱动反馈 DNA 电路,用于放大适体传感,例如三磷酸腺苷 (ATP) 和凝血酶,在活细胞中具有显著提高的灵敏度。该起始子复制杂交链式反应 (ID-HCR) 电路通过将 HCR 电路与 DNA 酶生物催化相结合而获得。此外,自动催化驱动的适体传感器由识别元件和放大元件组成。识别单元可以通过多功能构象转化特异性识别 ATP 或凝血酶,从而使起始子暴露于自动催化驱动电路。ID-HCR 元件集成了 HCR 的迷人自组装特性和 DNA 酶的显著催化裂解能力,以实现触发链的连续自我维持再生或复制,并实现指数信号增益。自动催化驱动的适体传感器已被验证用于体外定量分析 ATP 和凝血酶,并用于监测活细胞中具有各种表达的相应适体底物。更重要的是,作为一种通用的放大策略,自动催化驱动的适体传感器通过仅改变系统的识别元件,具有分析其他较少丰度生物标志物的巨大潜力。

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