FEBS Open Bio (Jan 2014)

Rational design of a structure-switching DNA aptamer for potassium ions

  • Andrew T. Catherine,
  • Stephanie N. Shishido,
  • Gregg A. Robbins-Welty,
  • Amy Diegelman-Parente

DOI
https://doi.org/10.1016/j.fob.2014.08.008
Journal volume & issue
Vol. 4, no. C
pp. 788 – 795

Abstract

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Structure-switching molecules provide a unique means for analyte detection, generating a response to analyte concentration through a binding-specific conformational change between non-binding and binding-competent states. While most ligand-binding molecules are not structure switching by default, many can be engineered to be so through the introduction of an alternative non-binding (and thus non-signalling) conformation. This population-shift mechanism is particularly effective with oligonucleotides and has led to the creation of structure-switching aptamers for many target ligands. Here, we report the rational design of structure-switching DNA aptamers, based on the thrombin binding aptamer (TBA), that bind potassium with affinities that bridge the gap between previously reported weak-binding and strong-binding aptamers. We also demonstrate a correlation between the free energy of the experimentally determined binding affinity for potassium and the computationally estimated free energy of the alternative (non-binding) structure.

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