Explore unprecedented binding sites on protein targets by screening #covalent heterocyclic MiniFrags. See how they work identifying novel #allosteric sites on HDAC8 https://is.gd/CdPLih
Thanks @EnamineLtd
for making the covalent MiniFrags available https://is.gd/7LN1sb
I always enjoy sharing Eline's work. She was a close collaborator during graduate school at UCSF.
With colleagues, Eline has extended the project we worked on together 5+ years ago and done the near-impossible: graft a covalent and non-covalent fragment into a PPI stabilizer.
Check it out!
https://onlinelibrary.wiley.com/doi/full/10.1002/anie.202308004
Really nice review just published on the use of covalently-bound fragments in #DrugDiscovery by some current and former colleagues #FBDD #Chemistry
Fragment based drug discovery has long been used for the identification of new ligands and interest in targeted covalent inhibitors has continued to grow in recent years, with high profile drugs such as osimertinib and sotorasib gaining FDA approval. It is therefore unsurprising that covalent fragment-based approaches have become popular and have recently led to the identification of novel targets and binding sites, as well as ligands for targets previously thought to be ‘undruggable’. Understanding the properties of such covalent fragments is important, and characterizing and/or predicting reactivity can be highly useful. This review aims to discuss the requirements for an electrophilic fragment library and the importance of differing warhead reactivity. Successful case studies from the world of drug discovery are then be examined.
RCNS MedChem Research Group
Ken Hallenbeck
JohnTaylor