AI Article Synopsis

  • The discovery of new scaffolds for selectively targeting RNA is crucial in medicinal chemistry, particularly for developing treatments for cancers linked to oncogenic miRNAs.
  • Researchers created a new series of RNA ligands derived from the 2-deoxystreptamine scaffold, which is a component of the aminoglycoside neomycin, to target the biogenesis of pre-miR-372, which is associated with cancer.
  • Some of these newly developed RNA ligands showed comparable biological activity to existing neomycin analogs, and their binding mechanisms with pre-miR-372 were investigated.

Article Abstract

The discovery of new original scaffolds for selective RNA targeting is one of the main challenges of current medicinal chemistry since therapeutically relevant RNAs represent potential targets for a number of pathologies. Recent efforts have been devoted to the search for RNA ligands targeting the biogenesis of oncogenic miRNAs whose overexpression has been directly linked to the development of various cancers. In this work, we developed a new series of RNA ligands for the targeting of oncogenic miRNA biogenesis based on the 2-deoxystreptamine scaffold. The latter is part of the aminoglycoside neomycin and is known to play an essential role in the RNA interaction of this class of RNA binders. 2-deoxystreptamine was thus conjugated to natural and artificial nucleobases to obtain new binders of the oncogenic miR-372 precursor (pre-miR-372). We identified some conjugates exhibiting a similar biological activity to previously synthesized neomycin analogs and studied their mode of binding with the target pre-miR-372.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC8942232PMC
http://dx.doi.org/10.1039/d1md00345cDOI Listing

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