DNA Nanostructure-based Interfacial engineering for PCR-free ultrasensitive electrochemical analysis of microRNA

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作者
Yanli Wen
Hao Pei
Ye Shen
Junjie Xi
Meihua Lin
Na Lu
Xizhong Shen
Jiong Li
Chunhai Fan
机构
[1] Laboratory of Physical Biology,Division of Chemistry and lonizing Radiation Measurement Technology
[2] Shanghai Institute of Applied Physics,undefined
[3] Chinese Academy of Sciences,undefined
[4] Suzhou Institute of Nano-tech and Nano-bionics,undefined
[5] Chinese Academy of Sciences,undefined
[6] Zhongshan Hospital,undefined
[7] Fudan University,undefined
[8] Shanghai Institute of Measurement and Testing Technology,undefined
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摘要
MicroRNAs (miRNAs) have been identified as promising cancer biomarkers due to their stable presence in serum. As an alternative to PCR-based homogenous assays, surface-based electrochemical biosensors offer great opportunities for low-cost, point-of-care tests (POCTs) of disease-associated miRNAs. Nevertheless, the sensitivity of miRNA sensors is often limited by mass transport and crowding effects at the water-electrode interface. To address such challenges, we herein report a DNA nanostructure-based interfacial engineering approach to enhance binding recognition at the gold electrode surface and drastically improve the detection sensitivity. By employing this novel strategy, we can directly detect as few as attomolar (<1, 000 copies) miRNAs with high single-base discrimination ability. Given that this ultrasensitive electrochemical miRNA sensor (EMRS) is highly reproducible and essentially free of prior target labeling and PCR amplification, we also demonstrate its application by analyzing miRNA expression levels in clinical samples from esophageal squamous cell carcinoma (ESCC) patients.
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