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用于精确细胞内长链非编码RNA成像的具有多位点识别和多信号输出功能的工程化DNA纳米器件

Engineering DNA Nanodevices with Multi-site Recognition and Multi-signal Output for Accurate Intracellular LncRNA Imaging.

作者信息

Tang Jing-Yi, Zhao Mei-Ling, Zhou Xue-Mei, Chai Ya-Qin, Yuan Ruo, Lei Yan-Mei, Zhuo Ying

机构信息

Key Laboratory of Luminescence Analysis and Molecular Sensing, Ministry of Education, Institute of Developmental Biology and Regenerative Medicine, College of Chemistry and Chemical Engineering, Southwest University, Chongqing 400715, China.

出版信息

Anal Chem. 2025 Feb 18;97(6):3378-3386. doi: 10.1021/acs.analchem.4c05353. Epub 2025 Feb 5.

DOI:10.1021/acs.analchem.4c05353
PMID:39907677
Abstract

Dynamic DNA nanodevices, known for their high programmability and controllability, are pivotal in intracellular biomarker imaging. However, these nanodevices often suffer from inadequate detection sensitivity and specificity due to limited cellular loading capacity and low signal feedback. Herein, we engineered an integrated ulti-site rcognition and ulti-signal utput of fou-leaf clover dnamic DNA nanodevice () that enables sensitive and accurate intracellular long noncoding RNA (lncRNA) imaging. MEMORY features one fluorophore (FAM)-modified cross-shaped structure as spatial-confinement scaffolds loaded with four identical quenchers (BHQ1)-modified recognition probes (), ensuring a low background signal initially. In the presence of target lncRNA, the multiple recognition sites of MEMORY facilitate hybridization with the target to selectively release the RPs, exposing the toehold region and outputting the green fluorescence (FAM) signal. Furthermore, the exposed toehold region can trigger efficient and rapid hybridization chain reaction (HCR) amplification, outputting the red fluorescence (Cy5) signal. MEMORY's multiple recognition sites increase the likelihood of target collisions, enhancing reaction efficiency, while its multi-signal output provides sequential feedback through FAM and Cy5, boosting overall signal intensity. With the lncRNA metastasis-related lung adenocarcinoma transcript 1 (MALAT1) as a detection model, MEMORY offers a linear detection range from 1 pM to 100 nM, with a limit of detection of 0.29 pM. We demonstrated that MEMORY can differentiate between normal and tumor cells based on intracellular MALAT1 imaging. This integrated DNA nanodevice will offer valuable tools for sensitive and accurate imaging of intracellular biomarkers.

摘要

动态DNA纳米器件以其高可编程性和可控性而闻名,在细胞内生物标志物成像中起着关键作用。然而,由于细胞负载能力有限和信号反馈低,这些纳米器件常常存在检测灵敏度和特异性不足的问题。在此,我们设计了一种四叶苜蓿动态DNA纳米器件(MEMORY),它具有集成的多位点识别和多信号输出功能,能够实现灵敏且准确的细胞内长链非编码RNA(lncRNA)成像。MEMORY具有一个荧光团(FAM)修饰的十字形结构作为空间限制支架,其上负载有四个相同的猝灭剂(BHQ1)修饰的识别探针(RPs),从而确保最初具有低背景信号。在存在靶标lncRNA的情况下,MEMORY的多个识别位点促进与靶标的杂交,选择性地释放RPs,暴露引发区域并输出绿色荧光(FAM)信号。此外,暴露的引发区域可触发高效且快速的杂交链式反应(HCR)扩增,输出红色荧光(Cy5)信号。MEMORY的多个识别位点增加了靶标碰撞的可能性,提高了反应效率,而其多信号输出通过FAM和Cy5提供顺序反馈,增强了整体信号强度。以lncRNA转移相关的肺腺癌转录本1(MALAT1)作为检测模型,MEMORY的线性检测范围为1 pM至100 nM,检测限为0.29 pM。我们证明MEMORY可以基于细胞内MALAT1成像区分正常细胞和肿瘤细胞。这种集成的DNA纳米器件将为细胞内生物标志物的灵敏且准确成像提供有价值的工具。

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