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Evolution of multivalent supramolecular assemblies of aptamers with target-defined spatial organization

Artem Kononenko, Vincenzo Caroprese, Yoan Duhoo, Cem Tekin, Maartje M. C. Bastings

2025Nature Nanotechnology16 citationsDOIOpen Access PDF

Abstract

Rapid identification of neutralizing molecules against new and mutating viruses is key to efficiently combating biorisk. Current binder identification techniques use a monovalent library of potential binders. Interestingly, proteins on pathogens are often homo-oligomeric-for example, the SARS-CoV-2 spike protein is a homotrimer. Here we describe a simple strategy, MEDUSA (multivalent evolved DNA-based supramolecular assembly), to evolve multivalent assemblies of aptamers with precise interligand spacing and three-fold symmetry, mirroring the geometric structure of many viral capsid proteins. MEDUSA allowed the selection of potent SARS-CoV-2 spike binders structurally distinct from any known aptamers. Decoupling the geometric and structural rigidity contributions toward selectivity made it possible to connect form to function, as demonstrated by the design of tunable fluorescent sensors. This approach offers a blueprint for targeting geometrically defined pathogen structures and developing rapid-response tools for emerging pathogens.

Topics & Concepts

AptamerComputational biologyCapsidSupramolecular chemistryNanotechnologyChemistryBiophysicsBiologyMoleculeMaterials scienceGeneticsGeneBiochemistryOrganic chemistryAdvanced biosensing and bioanalysis techniquesBacteriophages and microbial interactionsRNA and protein synthesis mechanisms
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