Hata Aaron N, Lybrand Terry P, Marnett Lawrence J, Breyer Richard M
Department of Pharmacology, Vanderbilt University School of Medicine, Nashville, TN 37232-2372, USA.
Mol Pharmacol. 2005 Mar;67(3):640-7. doi: 10.1124/mol.104.007971. Epub 2004 Nov 24.
The chemoattractant receptor-homologous molecule expressed on Th2 cells (CRTH2) receptor, a G protein-coupled receptor that mediates chemotaxis of inflammatory cells in response to prostaglandin D2 (PGD2), is hypothesized to play a role in Th2-mediated allergic disease. In addition to PGD2, CRTH2 can be activated by indomethacin, a nonselective cyclooxygenase inhibitor and widely used nonsteroidal anti-inflammatory drug (NSAID). To evaluate the structural features that confer CRTH2 binding selectivity, structure-activity relationship analysis of arylacetic acid class NSAIDs as CRTH2 receptor ligands was performed. Indomethacin, sulindac sulfide, and zomepirac displaced [3H]PGD2 binding at the mouse CRTH2 receptor (mCRTH2) with comparable affinity (Ki = 1.5 +/- 0.1, 2.5 +/- 0.4, and 3.3 +/- 0.3 microM, respectively). The indomethacin metabolite 5'-O-desmethyl indomethacin (5'-DMI) possessed binding affinity similar to indomethacin; however, elimination of the 2-methyl substituent on the indole ring resulted in a 10-fold decrease in binding affinity. No binding was detected for indole acetic acid and indole derivatives such as tryptophan, serotonin, and 5-hydroxy indole acetic acid, demonstrating the importance of the N-acyl moiety of indomethacin. Neutral derivatives of indomethacin also failed to bind to mCRTH2, suggesting that the negatively charged carboxylate moiety participates in a key ligand-receptor interaction. Despite similar binding affinities, NSAID-type mCRTH2 ligands exhibited variable potencies as mCRTH2 agonists. Sulindac sulfide and 5'-DMI inhibited intracellular cyclic AMP ([cAMP]i) generation and stimulated cell migration comparable with indomethacin. In contrast, zomepirac did not inhibit [cAMP]i generation or stimulate cell migration but weakly antagonized the effects of indomethacin on [cAMP]i. Together, these results reveal structural features of arylacetic acid NSAIDs that may be exploited for the development of selective CRTH2 ligands.
Th2细胞上表达的趋化因子受体同源分子(CRTH2)受体是一种G蛋白偶联受体,可介导炎症细胞对前列腺素D2(PGD2)产生趋化作用,据推测其在Th2介导的过敏性疾病中发挥作用。除PGD2外,CRTH2还可被吲哚美辛激活,吲哚美辛是一种非选择性环氧化酶抑制剂,也是广泛使用的非甾体抗炎药(NSAID)。为评估赋予CRTH2结合选择性的结构特征,对作为CRTH2受体配体的芳基乙酸类NSAIDs进行了构效关系分析。吲哚美辛、舒林酸硫化物和佐美酸以相当的亲和力(分别为Ki = 1.5±0.1、2.5±0.4和3.3±0.3 microM)取代小鼠CRTH2受体(mCRTH2)上的[3H]PGD2结合。吲哚美辛代谢物5'-O-去甲基吲哚美辛(5'-DMI)具有与吲哚美辛相似的结合亲和力;然而,吲哚环上2-甲基取代基的消除导致结合亲和力下降10倍。未检测到吲哚乙酸和吲哚衍生物如色氨酸、5-羟色胺和5-羟吲哚乙酸的结合,这表明吲哚美辛的N-酰基部分很重要。吲哚美辛中性衍生物也不能与mCRTH2结合,提示带负电荷的羧基部分参与关键的配体-受体相互作用。尽管结合亲和力相似,但NSAID型mCRTH2配体作为mCRTH2激动剂表现出不同的效力。舒林酸硫化物和5'-DMI抑制细胞内环状AMP([cAMP]i)生成并刺激细胞迁移,与吲哚美辛相当。相比之下,佐美酸不抑制[cAMP]i生成或刺激细胞迁移,但能微弱拮抗吲哚美辛对[cAMP]i的作用。总之,这些结果揭示了芳基乙酸类NSAIDs的结构特征,可用于开发选择性CRTH2配体。
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