Hanson Julien, Dogné Jean-Michel, Ghiotto Jérémie, Moray Anne-Lise, Kinsella B Therese, Pirotte Bernard
Drug Research Center, Laboratory of Medicinal Chemistry, University of Liège, 1 Avenue de l'Hôpital, B-4000 Liège, Belgium.
J Med Chem. 2007 Aug 9;50(16):3928-36. doi: 10.1021/jm070427h. Epub 2007 Jul 14.
The prostanoid thromboxane (TX)A2 exerts its proaggregant and constrictive actions upon binding to the specific TXA2 receptor (TP), a member of the G-protein coupled receptor superfamily. In humans, TXA2 signals through two distinct TP isoforms, TPalpha and TPbeta. Herein, we describe the design, synthesis, and SAR study of a series of original N-alkyl-N'-[2-(aryloxy)-5-nitrobenzenesulfonyl]ureas and -cyanoguanidine. The SAR study was based on the results of a functional assay, TP-mediated intracellular calcium ([Ca2+]i) mobilization performed on the two separate isoforms. Optimal nature and position of several structural moieties was defined for both activity and selectivity toward TPalpha and TPbeta isoforms. Three compounds (9h, 9af, and 9ag), showing increased selectivity for TPbeta relative to TPalpha (23.2:1, 18.1:1, 19.9:1, respectively), were selected for further experiments, and their activity was confirmed in a platelet aggregation assay. This study represents the first extended SAR study dealing with the identification of isoform selective antagonists for the human TXA2 receptor.
前列腺素血栓素(TX)A2与特异性TXA2受体(TP)结合后发挥其促聚集和收缩作用,TP是G蛋白偶联受体超家族的成员。在人类中,TXA2通过两种不同的TP亚型TPα和TPβ发出信号。在此,我们描述了一系列新型N-烷基-N'-[2-(芳氧基)-5-硝基苯磺酰基]脲和氰基胍的设计、合成及构效关系研究。构效关系研究基于在两种不同亚型上进行的功能性试验结果,即TP介导的细胞内钙([Ca2+]i)动员。确定了几个结构部分的最佳性质和位置,以实现对TPα和TPβ亚型的活性和选择性。选择了三种对TPβ相对于TPα具有更高选择性的化合物(9h、9af和9ag,选择性分别为23.2:1、18.1:1、19.9:1)进行进一步实验,并在血小板聚集试验中证实了它们的活性。这项研究代表了首次针对人类TXA2受体亚型选择性拮抗剂鉴定的扩展构效关系研究。
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