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Merck
  • A selective prostaglandin E2 receptor subtype 2 (EP2) antagonist increases the macrophage-mediated clearance of amyloid-beta plaques.

A selective prostaglandin E2 receptor subtype 2 (EP2) antagonist increases the macrophage-mediated clearance of amyloid-beta plaques.

Journal of medicinal chemistry (2015-06-11)
Brian M Fox, Hilary P Beck, Philip M Roveto, Frank Kayser, Qingwen Cheng, Hannah Dou, Toni Williamson, James Treanor, Hantao Liu, Lixia Jin, Guifen Xu, Ji Ma, Songli Wang, Steven H Olson
RESUMO

A high-throughput screen resulted in the discovery of benzoxazepine 1, an EP2 antagonist possessing low microsomal stability and potent CYP3A4 inhibition. Modular optimization of lead compound 1 resulted in the discovery of benzoxazepine 52, a molecule with single-digit nM binding affinity for the EP2 receptor and significantly improved microsomal stability. It was devoid of CYP inhibition and was ∼4000-fold selective against the other EP receptors. Compound 52 was shown to have good PK properties in CD-1 mice and high CNS permeability in C57Bl/6s mice and Sprague-Dawley rats. In an ex vivo assay, it demonstrated the ability to increase the macrophage-mediated clearance of amyloid-beta plaques from brain slices in a dose-dependent manner.

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Sigma-Aldrich
EP2 antagonist C52, ≥98% (HPLC)