| Literature DB >> 30449673 |
Amit Shraga1, Evgenia Olshvang1, Natalia Davidzohn2, Payam Khoshkenar3, Nicolas Germain4, Khriesto Shurrush4, Silvia Carvalho4, Liat Avram5, Shira Albeck6, Tamar Unger6, Bruce Lefker7, Chakrapani Subramanyam7, Robert L Hudkins8, Amir Mitchell3, Ziv Shulman2, Takayoshi Kinoshita9, Nir London10.
Abstract
The c-Jun NH2-terminal kinase (JNK) signaling pathway is central to the cell response to stress, inflammatory signals, and toxins. While selective inhibitors are known for JNKs and for various upstream MAP3Ks, no selective inhibitor is reported for MKK7--one of two direct MAP2Ks that activate JNK. Here, using covalent virtual screening, we identify selective MKK7 covalent inhibitors. We optimized these compounds to low-micromolar inhibitors of JNK phosphorylation in cells. The crystal structure of a lead compound bound to MKK7 demonstrated that the binding mode was correctly predicted by docking. We asserted the selectivity of our inhibitors on a proteomic level and against a panel of 76 kinases, and validated an on-target effect using knockout cell lines. Lastly, we show that the inhibitors block activation of primary mouse B cells by lipopolysaccharide. These MKK7 tool compounds will enable better investigation of JNK signaling and may serve as starting points for therapeutics.Entities:
Keywords: DOCKovalent; JNK; MAPK; MKK7; covalent docking; covalent inhibitor; kinase inhibitors; virtual screening
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Year: 2018 PMID: 30449673 DOI: 10.1016/j.chembiol.2018.10.011
Source DB: PubMed Journal: Cell Chem Biol ISSN: 2451-9448 Impact factor: 8.116