X-ray Screening of an Electrophilic Fragment Library and Application toward the Development of a Novel ERK 1/2 Covalent Inhibitor.
Jeffrey D St DenisGianni ChessariAnne CleasbyBenjamin D ConsSuzanna CowanSamuel E DaltonCharlotte EastChristopher W MurrayMarc O'ReillyTorren PeakmanMagdalini RaptiJessie L StowPublished in: Journal of medicinal chemistry (2022)
Fragment-based drug discovery (FBDD) has become an established method for the identification of efficient starting points for drug discovery programs. In recent years, electrophilic fragment screening has garnered increased attention from both academia and industry to identify novel covalent hits for tool compound or drug development against challenging drug targets. Herein, we describe the design and characterization of an acrylamide-focused electrophilic fragment library and screening campaign against extracellular signal-regulated kinase 2 (ERK2) using high-throughput protein crystallography as the primary hit-finding technology. Several fragments were found to have covalently modified the adenosine triphosphate (ATP) binding pocket Cys166 residue. From these hits, 22 , a covalent ATP-competitive inhibitor with improved potency (ERK2 IC 50 = 7.8 μM), was developed.
Keyphrases
- drug discovery
- signaling pathway
- high throughput
- cell proliferation
- pi k akt
- public health
- high resolution
- transcription factor
- binding protein
- working memory
- amino acid
- computed tomography
- protein kinase
- emergency department
- small molecule
- tyrosine kinase
- mass spectrometry
- dna binding
- drug induced
- electron microscopy