Litcius/Paper detail

Efficient NMR Screening Approach to Discover Small Molecule Fragments Binding Structured RNA

Matthew D. Shortridge, Gabriele Varani

2021ACS Medicinal Chemistry Letters21 citationsDOIOpen Access PDF

Abstract

We describe a scalable nuclear magnetic resonance (NMR) screening approach to identify and prioritize small molecule fragments that bind to structured RNAs. This approach is target agnostic and, therefore, amenable to many RNA structures and libraries, and it provides initial hits for further synthetic elaboration and structure-based drug discovery efforts. We demonstrate the approach on the pre-miR-21 stem-loop, which is of significant interest in oncology and metabolic diseases. We screened the pre-miR-21 hairpin using a small (420 compounds) commercially available fragment library and identified 18 hits in the first round of triage screening. This was further refined to four fragments which passed all screening cascade filters. Among these four hits, a thiadiazole fragment was demonstrated to bind the Dicer cleavage site of pre-miR-21 by target-detected NMR experiments and through the observation of clear intermolecular NOEs.

Topics & Concepts

Small moleculeComputational biologyRNAStem-loopFragment (logic)Drug discoveryDicerChemistryCombinatorial chemistryStereochemistryBiologyComputer scienceBiochemistryRNA interferenceGeneProgramming languageRNA modifications and cancerRNA and protein synthesis mechanismsRNA Research and Splicing
Efficient NMR Screening Approach to Discover Small Molecule Fragments Binding Structured RNA | Litcius