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Discovery and Optimization of a Novel Series of Highly Selective JAK1 Kinase Inhibitors.

Neil P GrimsterErica AndersonMarat AlimzhanovGeraldine BebernitzKirsten BellClaudio ChuaquiTracy DeeganAndrew D FergusonThomas GeroAndreas HarschDennis HuszarAarti KawatkarJason G KettlePaul LyneJon A ReadCaroline Rivard CostaLinette RustonPatricia SchroederJie ShiQibin SuScott ThronerDorin ToaderMelissa VasbinderRichard WoessnerHaixia WangAllan WuMinwei YeWeijia ZhengMichael Zinda
Published in: Journal of medicinal chemistry (2018)
Janus kinases (JAKs) have been demonstrated to be critical in cytokine signaling and have thus been implicated in both cancer and inflammatory diseases. The JAK family consists of four highly homologous members: JAK1-3 and TYK2. The development of small-molecule inhibitors that are selective for a specific family member would represent highly desirable tools for deconvoluting the intricacies of JAK family biology. Herein, we report the discovery of a potent JAK1 inhibitor, 24, which displays ∼1000-fold selectivity over the other highly homologous JAK family members (determined by biochemical assays), while also possessing good selectivity over other kinases (determined by panel screening). Moreover, this compound was demonstrated to be orally bioavailable and possesses acceptable pharmacokinetic parameters. In an in vivo study, the compound was observed to dose dependently modulate the phosphorylation of STAT3 (a downstream marker of JAK1 inhibition).
Keyphrases
  • small molecule
  • high throughput
  • dna damage
  • oxidative stress
  • cell proliferation
  • squamous cell carcinoma
  • papillary thyroid
  • protein kinase
  • structural basis