| Literature DB >> 29348070 |
Frank Lovering1, Paul Morgan2, Christophe Allais3, Ann Aulabaugh3, Joanne Brodfuehrer4, Jeanne Chang3, Jotham Coe3, WeiDong Ding3, Heather Dowty5, Margaret Fleming2, Richard Frisbie3, Julia Guzova2, David Hepworth6, Jayasankar Jasti3, Steve Kortum3, Ravi Kurumbail3, Shashi Mohan2, Nikolaos Papaioannou6, Joseph W Strohbach6, Fabien Vincent3, Katherine Lee6, Christoph W Zapf6.
Abstract
Many diseases are believed to be driven by pathological levels of reactive oxygen species (ROS) and oxidative stress has long been recognized as a driver for inflammatory disorders. Apoptosis signal-regulating kinase 1 (ASK1) has been reported to be activated by intracellular ROS and its inhibition leads to a down regulation of p38-and JNK-dependent signaling. Consequently, ASK1 inhibitors may have the potential to treat clinically important inflammatory pathologies including renal, pulmonary and liver diseases. Analysis of the ASK1 ATP-binding site suggested that Gln756, an amino acid that rarely occurs at the GK+2 position, offered opportunities for achieving kinase selectivity for ASK1 which was applied to the design of a parallel medicinal chemistry library that afforded inhibitors of ASK1 with nanomolar potency and excellent kinome selectivity. A focused optimization strategy utilizing structure-based design resulted in the identification of ASK1 inhibitors with low nanomolar potency in a cellular assay, high selectivity when tested against kinase and broad pharmacology screening panels, and attractive physicochemical properties. The compounds we describe are attractive tool compounds to inform the therapeutic potential of ASK1 inhibition.Entities:
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Year: 2017 PMID: 29348070 DOI: 10.1016/j.ejmech.2017.12.041
Source DB: PubMed Journal: Eur J Med Chem ISSN: 0223-5234 Impact factor: 6.514