Inverse agonist activity of pirenzepine at M2 muscarinic acetylcholine receptors

被引:18
|
作者
Daeffler, L [1 ]
Schmidlin, F [1 ]
Gies, JP [1 ]
Landry, Y [1 ]
机构
[1] Univ Strasbourg 1, Fac Pharm, INSERM, U425,Lab Neuroimmunopharmacol, F-67401 Illkirch Graffenstaden, France
关键词
inverse agonism; muscarinic M-2 receptors; G protein; pirenzepine; mastoparan; GPAnt-2; GppNHp;
D O I
10.1038/sj.bjp.0702407
中图分类号
R9 [药学];
学科分类号
1007 ;
摘要
1 The intrinsic properties of muscarinic ligands were studied through their binding properties and their abilities to modulate the GTPase activity of G proteins coupled to muscarinic M-2 receptors in pig atrial sarcolemma. 2 Competition binding experiments were performed with [H-3]-oxotremorine-M to assess the affinity of receptors coupled to G proteins (R*), with [H-3]-N-methylscopolamine ([H-3]-NMS) to estimate the affinities of coupled and uncoupled receptors (R*+R) and with [H-3]-NMS in the presence of GppNHp to assess the affinity of uncoupled receptors (R). 3 The ranking of K-i values for the agonist carbachol was R*<<R*+R<<R (0.95, 124 and 1017 nM). K-i values for atropine and AF-DX 116 were similar for the three binding conditions (0.34, 0.42, 0.41 and 19, 22, 32 nM). The ranking of K-i values for pirenzepine was R*>R*+R>R (174, 155, 115 nM), suggesting inverse agonism. 4 The V-max of the basal high affinity GTPase activity of pig atrial sarcolemma was increased by mastoparan and decreased by GPAnt-2 indicating the relevance of this activity to G proteins coupled to receptors (R*). The K-M value (0.26-0.33 mu M) was not modified by mastoparan or GPAnt-2. 5 Carbachol increased the V-max of GTP hydrolysis (EC50 8.1+/-0.3 mu M), whereas atropine and AF-DX 116, up to 1 mM, did not modify it. Pirenzepine decreased the V-max of GTP hydrolysis (EC50 77.5+/-10.3 mu M). This effect was enhanced when KCl was substituted for NaCl (EC50 11.0+/-0.8 mu M) and was antagonized by atropine and AF-DX 116 (IC50 0.91+/-0.71 and 197+/-85 nM). 6 Pirenzepine is proposed as an inverse agonist and atropine and AF-DX 116 as neutral antagonists at the muscarinic M-2 receptor.
引用
收藏
页码:1246 / 1252
页数:7
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