DNAzyme-based faithful probing and pulldown to identify candidate biomarkers of low abundance

Nat Chem. 2024 Jan;16(1):122-131. doi: 10.1038/s41557-023-01328-5. Epub 2023 Sep 14.

Abstract

Biomarker discovery is essential for the understanding, diagnosis, targeted therapy and prognosis assessment of malignant diseases. However, it remains a huge challenge due to the lack of sensitive methods to identify disease-specific rare molecules. Here we present MORAC, molecular recognition based on affinity and catalysis, which enables the effective identification of candidate biomarkers with low abundance. MORAC relies on a class of DNAzymes, each cleaving a sole RNA linkage embedded in their DNA chain upon specifically sensing a complex system with no prior knowledge of the system's molecular content. We show that signal amplification from catalysis ensures the DNAzymes high sensitivity (for target probing); meanwhile, a simple RNA-to-DNA mutation can shut down their RNA cleavage ability and turn them into a pure affinity tool (for target pulldown). Using MORAC, we identify previously unknown, low-abundance candidate biomarkers with clear clinical value, including apolipoprotein L6 in breast cancer and seryl-tRNA synthetase 1 in polyps preceding colon cancer.

MeSH terms

  • Biomarkers
  • Biosensing Techniques*
  • DNA
  • DNA, Catalytic* / genetics
  • RNA

Substances

  • DNA, Catalytic
  • DNA
  • RNA
  • Biomarkers