4.8 Article

Interfacial DNA Framework-Enhanced Background-to-Signal Transition for Ultrasensitive and Specific Micro-RNA Detection

Journal

ACS APPLIED MATERIALS & INTERFACES
Volume 14, Issue 16, Pages 18209-18218

Publisher

AMER CHEMICAL SOC
DOI: 10.1021/acsami.2c03075

Keywords

DNA framework; electrochemistry; circulating microRNAs; polyaniline; diagnostics

Funding

  1. National Natural Science Foundation of China [21974037, 21775034, 82060647]
  2. Natural Science Foundation of Guangxi [2021GXNSFFA220003, 2021JJD120048]
  3. Guangxi Medical University Training Program for Distinguished Young Scholars
  4. Guangxi key R D Project [Guike AB18050008]
  5. Guangxi Science and Technology Program (Guike Jizi [2020]) [198]

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In this study, a DNA framework-reversed signal-gain strategy was developed to improve the signal-to-noise ratio in charge-based electrochemical DNA sensors for ultrasensitive and highly specific electrical detection of microRNAs (miRNAs) in blood. The DNA framework-based electrochemical sensor exhibited high sensitivity and specificity, allowing for the detection of tumor-associated miRNAs in complex matrices and the differentiation of tumor patients from normal individuals.
Interfacial DNA self-assembly is fundamental to solid nucleic acid biosensors, whereas how to improve the signal-to-noise ratio has always been a challenge, especially in the charge-based electrochemical DNA sensors because of the large noise from the negatively charged DNA capture probes. Here, we report a DNA framework-reversed signal-gain strategy through background-to-signal transition for ultrasensitive and highly specific electrical detection of microRNAs (miRNAs) in blood. By using a model of enzymecatalyzed deposition of conductive molecules (polyaniline) targeting to DNA, we observed the highest signal contribution per unit area by the highly charged three-dimensional (3D) tetrahedral DNA framework probe, relative to the modest of two-dimensional (2D) polyA probe and the lowest of onedimensional (1D) single-stranded (ss)DNA probe, suggesting the positive correlation of background DNA charge with signal enhancement. Using such an effective signal-transition design, the DNA framework-based electrochemical sensor achieves ultrasensitive miRNAs detection with sensitivity up to 0.29 fM (at least 10-fold higher than that with 1D ssDNA or 2D polyA probes) and high specificity with single-base resolution. More importantly, this high-performance sensor allows for a generalized sandwich detection of tumor-associated miRNAs in the complex matrices (multiple cell lysates and blood serum) and further distinguishes the tumor patients (e.g., breast, lung, and liver cancer) from the normal individuals. These advantages signify the promise of this miRNA sensor as a versatile tool in precision diagnosis.

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