Adventures in Scaffold Morphing: Discovery of Fused Ring Heterocyclic Checkpoint Kinase 1 (CHK1) Inhibitors.
Bin YangMelissa M VasbinderAlexander W HirdQibin SuHaixia WangYan YuDorin ToaderPaul D LyneJon A ReadJason BreedStephanos IoannidisChun DengMichael GrondineNancy DeGraceDavid WhitstonPatrick BrassilJames W JanetkaPublished in: Journal of medicinal chemistry (2018)
Checkpoint kinase 1 (CHK1) inhibitors are potential cancer therapeutics that can be utilized for enhancing the efficacy of DNA damaging agents. Multiple small molecule CHK1 inhibitors from different chemical scaffolds have been developed and evaluated in clinical trials in combination with chemotherapeutics and radiation treatment. Scaffold morphing of thiophene carboxamide ureas (TCUs), such as AZD7762 (1) and a related series of triazoloquinolines (TZQs), led to the identification of fused-ring bicyclic CHK1 inhibitors, 7-carboxamide thienopyridines (7-CTPs), and 7-carboxamide indoles. X-ray crystal structures reveal a key intramolecular noncovalent sulfur-oxygen interaction in aligning the hinge-binding carboxamide group to the thienopyridine core in a coplanar fashion. An intramolecular hydrogen bond to an indole NH was also effective in locking the carboxamide in the preferred bound conformation to CHK1. Optimization on the 7-CTP series resulted in the identification of lead compound 44, which displayed respectable drug-like properties and good in vitro and in vivo potency.
Keyphrases
- small molecule
- dna damage response
- clinical trial
- dna damage
- tissue engineering
- cell cycle
- emergency department
- high resolution
- papillary thyroid
- tyrosine kinase
- genome wide
- high throughput
- randomized controlled trial
- cell proliferation
- radiation therapy
- single cell
- single molecule
- climate change
- binding protein
- bioinformatics analysis
- combination therapy
- cell free
- study protocol
- crystal structure
- energy transfer
- quantum dots
- placebo controlled