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Discovery of E3 Ligase Ligands for Target Protein Degradation.

Jaeseok LeeYoungjun LeeYoung-Mee JungJu Hyun ParkHyuk Sang YooJongmin Park
Published in: Molecules (Basel, Switzerland) (2022)
Target protein degradation has emerged as a promising strategy for the discovery of novel therapeutics during the last decade. Proteolysis-targeting chimera (PROTAC) harnesses a cellular ubiquitin-dependent proteolysis system for the efficient degradation of a protein of interest. PROTAC consists of a target protein ligand and an E3 ligase ligand so that it enables the target protein degradation owing to the induced proximity with ubiquitin ligases. Although a great number of PROTACs has been developed so far using previously reported ligands of proteins for their degradation, E3 ligase ligands have been mostly limited to either CRBN or VHL ligands. Those PROTACs showed their limitation due to the cell type specific expression of E3 ligases and recently reported resistance toward PROTACs with CRBN ligands or VHL ligands. To overcome these hurdles, the discovery of various E3 ligase ligands has been spotlighted to improve the current PROTAC technology. This review focuses on currently reported E3 ligase ligands and their application in the development of PROTACs.
Keyphrases
  • small molecule
  • protein protein
  • binding protein
  • amino acid
  • high throughput
  • poor prognosis
  • oxidative stress
  • drug delivery
  • endothelial cells
  • long non coding rna
  • cancer therapy
  • diabetic rats
  • stress induced