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Proteolysis-targeting chimeras in drug development: A safety perspective.

Kevin MoreauMuireann CoenAndrew X ZhangFiona PachlM Paola CastaldiGoran DahlHelen BoydClay ScottPete Newham
Published in: British journal of pharmacology (2020)
Proteolysis-targeting chimeras are a new drug modality that exploits the endogenous ubiquitin proteasome system to degrade a protein of interest for therapeutic benefit. As the first-generation of proteolysis-targeting chimeras have now entered clinical trials for oncology indications, it is timely to consider the theoretical safety risks inherent with this modality which include off-target degradation, intracellular accumulation of natural substrates for the E3 ligases used in the ubiquitin proteasome system, proteasome saturation by ubiquitinated proteins, and liabilities associated with the "hook effect" of proteolysis-targeting chimeras This review describes in vitro and non-clinical in vivo data that provide mechanistic insight of these safety risks and approaches being used to mitigate these risks in the next generation of proteolysis-targeting chimera molecules to extend therapeutic applications beyond life-threatening diseases.
Keyphrases
  • cancer therapy
  • clinical trial
  • human health
  • small molecule
  • emergency department
  • palliative care
  • risk assessment
  • big data
  • climate change
  • artificial intelligence