A highly selective purine-based inhibitor of CSF1R potently inhibits osteoclast differentiation
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https://hdl.handle.net/10037/29242Date
2023-04-28Type
Journal articleTidsskriftartikkel
Peer reviewed
Author
Aarhus, Thomas Ihle; Eickhoff, Jan; Klebl, Bert; Unger, Anke; Boros, Johanna; Choidas, Axel; Zischinsky, Mia-Lisa; Wolowczyk, Camilla Izabel; Bjørkøy, Geir; Sundby, Eirik; Hoff, Bård HelgeAbstract
The colony-stimulating factor 1 receptor (CSF1R) plays an important role in the regulation of many inflammatory
processes, and overexpression of the kinase is implicated in several disease states. Identifying selective, smallmolecule inhibitors of CSF1R may be a crucial step toward treating these disorders. Through modelling, synthesis, and a systematic structure-activity relationship study, we have identified a number of potent and highly
selective purine-based inhibitors of CSF1R. The optimized 6,8-disubstituted antagonist, compound 9, has
enzymatic IC50 of 0.2 nM, and displays a strong affinity toward the autoinhibited form of CSF1R, contrasting that
of other previously reported inhibitors. As a result of its binding mode, the inhibitor shows excellent selectivity
(Selectivity score: 0.06), evidenced by profiling towards a panel of 468 kinases. In cell-based assays, this inhibitor
shows dose-dependent blockade of CSF1-mediated downstream signalling in murine bone marrow-derived
macrophages (IC50 = 106 nM) as well as disruption of osteoclast differentiation at nanomolar levels. In vivo
experiments, however, indicate that improve metabolic stability is needed in order to further progress this
compound class.
Publisher
ElsevierCitation
Aarhus TI, Eickhoff J, Klebl B, Unger A, Boros, Choidas A, Zischinsky M, Wolowczyk CI, Bjørkøy GB, Sundby E, Hoff BH. A highly selective purine-based inhibitor of CSF1R potently inhibits osteoclast differentiation. European Journal of Medicinal Chemistry. 2023;255:115344Metadata
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