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光激活和自驱动自主 DNA 纳米机器,实现活细胞中 microRNA 的荧光成像,具有卓越的精度和效率。

Light-Activated and Self-Driven Autonomous DNA Nanomachine Enabling Fluorescence Imaging of MicroRNA in Living Cells with Exceptional Precision and Efficiency.

机构信息

Hubei Province Key Laboratory of Occupational Hazard Identification and Control, School of Public Health, Medical College, Wuhan University of Science and Technology, Wuhan 430065, People's Republic of China.

College of Chemistry and Molecular Sciences, Wuhan University, Wuhan 430072, People's Republic of China.

出版信息

ACS Appl Mater Interfaces. 2021 Jul 14;13(27):31485-31494. doi: 10.1021/acsami.1c07333. Epub 2021 Jun 29.

DOI:10.1021/acsami.1c07333
PMID:34184527
Abstract

Owing to their favorable design flexibility and eminent signal amplification ability, DNA nanomachine-supported biosensors have provided an attractive avenue for intracellular fluorescence imaging, especially for DNA walkers. However, this promising option not only suffers from poor controllability but also needs to be supplied with additional driving forces on account of the frequent employment of metal ion-dependent DNAzymes. Aiming at overcoming these obstacles, we introduce some fruitful solutions. On one hand, innovative light-activated walking behavior induced by a photocleavage mode is established on the surfaces of gold nanoparticles, and such a photoselective sensing system can be perfectly prevented from pre-activating during the intracellular delivery process and made to achieve target identification only under irradiation using a moderate ultraviolet light source. On the other hand, this light-switchable sensing frame is encapsulated within a dissociable metal-organic framework (ZIF-8) to facilitate endocytosis and ensure sufficient internal cofactors (Zn) to realize a self-driven pattern in the acidic environment of the cell lysosome. Based on the abovementioned efforts, the newly constructed autonomous three-dimensional DNA walkers present satisfactory sensitivity (a limit of detection of down to 19.4 pM) and specificity (even distinguishing single-base changes) toward a model biomarker (microRNA-21). More importantly, the sensing method allows determination of the variations in targets in living cancer cells with exceptional precision and efficiency, offering a powerful assay platform for intracellular imaging.

摘要

由于其设计灵活性好和信号放大能力强,DNA 纳米机器支持的生物传感器为细胞内荧光成像提供了一种有吸引力的途径,特别是对于 DNA walker 而言。然而,这种很有前途的选择不仅受到较差的可控性的限制,而且由于频繁使用依赖金属离子的 DNA 酶,还需要额外的驱动力。针对这些障碍,我们引入了一些有效的解决方案。一方面,在金纳米粒子表面建立了一种由光催化断裂模式诱导的创新的光激活行走行为,并且这种光选择性传感系统可以在细胞内递呈过程中完全防止预先激活,并仅在使用适度的紫外光源照射下实现目标识别。另一方面,这个光开关传感框架被封装在可分离的金属有机骨架 (ZIF-8) 中,以促进内吞作用,并确保在细胞溶酶体的酸性环境中有足够的内部辅助因子 (Zn) 来实现自驱动模式。基于上述努力,新构建的自主式三维 DNA walker 对模型生物标志物 (microRNA-21) 具有令人满意的灵敏度 (低至 19.4 pM 的检测限) 和特异性 (甚至可以区分单个碱基变化)。更重要的是,该传感方法可以在活的癌细胞中以出色的精度和效率来确定靶标变化,为细胞内成像提供了强大的分析平台。

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