4.5 Review

Small molecule targeting of biologically relevant RNA tertiary and quaternary structures

Journal

CELL CHEMICAL BIOLOGY
Volume 28, Issue 5, Pages 594-609

Publisher

CELL PRESS
DOI: 10.1016/j.chembiol.2021.03.003

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Funding

  1. Duke University
  2. US National Institutes of Health [R35 GM124785]

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The development of small molecule ligands for non-coding RNAs shows therapeutic potential, with recent advances in technique enabling the identification of complex RNA structures and the design of selective molecules. Targeting RNA tertiary and quaternary structures with small molecules presents promising opportunities for treating human diseases.
Initial successes in developing small molecule ligands for non-coding RNAs have underscored their potential as therapeutic targets. More recently, these successes have been aided by advances in biophysical and structural techniques for identification and characterization of more complex RNA structures; these higher-level folds present protein-like binding pockets that offer opportunities to design small molecules that could achieve a degree of selectivity often hard to obtain at the primary and secondary structure level. More specifically, identification and small molecule targeting of RNA tertiary and quaternary structures have allowed researchers to probe several human diseases and have resulted in promising clinical candidates. In this review we highlight a selection of diverse and exciting successes and the experimental approaches that led to their discovery. These studies include examples of recent developments in RNA-centric assays and ligands that provide insight into the features responsible for the affinity and biological outcome of RNA-targeted chemical probes. This report highlights the potential and emerging opportunities to selectively target RNA tertiary and quaternary structures as a route to better understand and, ultimately, treat many diseases.

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