2024 article

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Exploring the Landscape of Aptamers: From Cross-Reactive to Selective to Specific, High-Affinity Receptors for Cocaine

Yang, K., Alkhamis, O., Canoura, J., Bryant, A., Gong, E. M., Barbu, M., … Landry, D. W. (2024, February 13). JACS AU.

By: K. Yang ^*, O. Alkhamis ⁿ, J. Canoura ⁿ, A. Bryant ⁿ, E. Gong^*, M. Barbu^*, S. Taylor ^*, D. Nikic^* ...and 4 other authors, including 1 NC State author, S. Banerjee ^*, Y. Xiao ⁿ , M. Stojanovic ^* & D. Landry ^*

author keywords: cocaine; aptamer; specific; high-affinity; cross-reactive; hydrophobic receptor

TL;DR: A series of progressively improved DNA aptamers recognizing cocaine are reported, with the final optimized receptors having low nanomolar affinity and over a thousand-fold selectivity over the initial cross-reactants. (via Semantic Scholar)

10.1021/jacsau.3c00781

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UN Sustainable Development Goal Categories

3. Good Health and Well-being (OpenAlex)

Source: Web Of Science

Added: March 11, 2024

We reported over 20 years ago MNS-4.1, the first DNA aptamer with a micromolar affinity for cocaine. MNS-4.1 is based on a structural motif that is very common in any random pool of oligonucleotides, and it is actually a nonspecific hydrophobic receptor with wide cross-reactivity with alkaloids and steroids. Despite such weaknesses preventing broad applications, this aptamer became widely used in proof-of-concept demonstrations of new formats of biosensors. We now report a series of progressively improved DNA aptamers recognizing cocaine, with the final optimized receptors having low nanomolar affinity and over a thousand-fold selectivity over the initial cross-reactants. In the process of optimization, we tested different methods to eliminate cross-reactivities and improve affinity, eventually achieving properties that are comparable to those of the reported monoclonal antibody candidates for the therapy of overdose. Multiple aptamers that we now report share structural motifs with the previously reported receptor for serotonin. Further mutagenesis studies revealed a palindromic, highly adaptable, broadly cross-reactive hydrophobic motif that could be rebuilt through mutagenesis, expansion of linker regions, and selections into receptors with exceptional affinities and varying specificities.