4.6 Article

Detection of urinary microRNA biomarkers using diazo sulfonamide-modified screen printed carbon electrodes

期刊

RSC ADVANCES
卷 11, 期 31, 页码 18832-18839

出版社

ROYAL SOC CHEMISTRY
DOI: 10.1039/d0ra09874d

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资金

  1. Wellcome Trust
  2. BBSRC [BB/K012592/1]
  3. Kidney Research UK [RP44/2014]
  4. Cardiff University
  5. Wales Kidney Research Unit
  6. BBSRC [BB/K012592/1] Funding Source: UKRI

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This paper introduces a straightforward electrochemical method for quantifying urinary miRNA using disposable biosensors to distinguish between DKD patients and control subjects. Aberrant miRNA expression has been observed in several major human disorders, and a urinary miRNA signature for DKD has been identified. The method shows great clinical and commercial potential for quantitative miRNA detection in liquid biopsies and may serve as a platform for non-invasive high-throughput screening.
This paper describes a straightforward electrochemical method for rapid and robust urinary microRNA (miRNA) quantification using disposable biosensors that can discriminate between urine from diabetic kidney disease (DKD) patients and control subjects. Aberrant miRNA expression has been observed in several major human disorders, and we have identified a urinary miRNA signature for DKD. MiRNAs therefore have considerable promise as disease biomarkers, and techniques to quantify these transcripts from clinical samples have significant clinical and commercial potential. Current RT-qPCR-based methods require technical expertise, and more straightforward methods such as electrochemical detection offer attractive alternatives. We describe a method to detect urinary miRNAs using diazo sulfonamide-modified screen printed carbon electrode-based biosensors that is amenable to parallel analysis. These sensors showed a linear response to buffered miR-21, with a 17 fM limit of detection, and successfully discriminated between urine samples (n = 6) from DKD patients and unaffected control subjects (n = 6) by differential miR-192 detection. Our technique for quantitative miRNA detection in liquid biopsies has potential for development as a platform for non-invasive high-throughput screening and/or to complement existing diagnostic procedures in disorders such as DKD.

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