Giblin Gerard M P, Bit Rino A, Brown Susan H, Chaignot Hélène M, Chowdhury Anita, Chessell Iain P, Clayton Nicholas M, Coleman Tanya, Hall Adrian, Hammond Beverley, Hurst David N, Michel Anton D, Naylor Alan, Novelli Riccardo, Scoccitti Tiziana, Spalding David, Tang Sac P, Wilson Alex W, Wilson Rich
Department of Medicinal Chemistry and DMPK, New Frontiers Science Park, Third Avenue, Harlow, Essex CM19 5AW, UK.
Bioorg Med Chem Lett. 2007 Jan 15;17(2):385-9. doi: 10.1016/j.bmcl.2006.10.041. Epub 2006 Oct 20.
The discovery of a series of selective EP1 receptor antagonists based on a 1,2-diarylcyclopentene template is described. After defining the structural requirements for EP1 potency and selectivity, heterocyclic rings were incorporated to reduce logD and improve in vitro pharmacokinetic properties. The 2,6-substituted pyridines and pyridazines gave an appropriate balance of potency, in vivo pharmacokinetic properties and a low potential for inhibiting a range of CYP450 enzymes. From this series, GW848687X was shown to have an excellent profile in models of inflammatory pain and was selected as a development candidate.
本文描述了基于1,2-二芳基环戊烯模板的一系列选择性EP1受体拮抗剂的发现。在确定了EP1活性和选择性的结构要求后,引入杂环以降低logD并改善体外药代动力学性质。2,6-取代的吡啶和哒嗪在活性、体内药代动力学性质以及抑制一系列CYP450酶的低可能性之间提供了适当的平衡。从该系列中,GW848687X在炎性疼痛模型中显示出优异的特性,并被选为开发候选物。
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