甲氧卡明与辛巴辛在体外对心房、平滑肌和内皮毒蕈碱受体的相互作用。
The interaction of methoctramine and himbacine at atrial, smooth muscle and endothelial muscarinic receptors in vitro.
作者信息
Eglen R M, Montgomery W W, Dainty I A, Dubuque L K, Whiting R L
机构信息
Institute of Pharmacology, Syntex Research, Palo Alto, CA 94304.
出版信息
Br J Pharmacol. 1988 Dec;95(4):1031-8. doi: 10.1111/j.1476-5381.1988.tb11736.x.
Abstract
- The action of methoctramine and himbacine at muscarinic receptors has been studied using guinea-pig isolated trachea, oesophageal muscularis mucosae, paced left atria, and rat aortic preparations. 2. Methoctramine (1 x 10(-6)-3.2 x 10(-4) M), but not himbacine, elicited positive inotropic responses. These responses were enhanced by pretreating the animals with reserpine. The responses in reserpine-treated animals were not antagonized by phentolamine (1 x 10(-6) M) but were antagonized by propranolol (1 x 10(-6) M). 3. Methoctramine, but not himbacine, exhibited allosteric inhibitory effects at cardiac muscarinic receptors, resulting in a curvilinear Schild plot. Deviations from competitive antagonism were also observed in combination dose-ratio experiments using atropine and methoctramine. At 1 x 10(-6) M, the pKB value for methoctramine was 7.88 +/- 0.15 (mean +/- s.e.mean, n = 5). The pA2 value for himbacine at cardiac muscarinic receptors was 8.52 +/- 0.06 (n = 3). 4. At tracheal and oesophageal muscularis mucosal smooth muscle receptors, the Schild plots for both antagonists were linear. The pA2 values for methoctramine at receptors in these two preparations were similar (6.08 +/- 0.05 and 6.03 +/- 0.09 respectively, n = 4) and were approximately 60 fold less than those values observed at atrial receptors. Himbacine, also exhibited similar values at muscarinic receptors in the trachea and oesophageal muscularis mucosae (7.61 +/- 0.05 and 7.57 +/- 0.04 respectively, n = 4). 5. Muscarinic receptors mediating relaxation of the rat aortic endothelium exhibited pA2 values for methoctramine (5.87 +/- 0.12, n = 6) which were similar to those observed in the smooth muscle, but not the atria. The pA2 values for himbacine at endothelial muscarinic receptors were approximately 0.5 pA2 units lower than those observed at muscarinic receptors in smooth muscle (6.92 + 0.80, n = 6). In addition, the Schild slopes for methoctramine and himbacine at these receptors were significantly (P < 0.05) less than unity. 6. Methoctramine, and to a lesser extent himbacine, are potent and selective antagonists for cardiac muscarinic receptors. However, caution should be used in interpretation of the data with methoctramine in view of the inhibitory allosteric properties and direct inotropic actions of this compound.
摘要
- 已使用豚鼠离体气管、食管肌层黏膜、起搏左心房和大鼠主动脉制剂研究了甲溴辛托品和辛巴生在毒蕈碱受体上的作用。2. 甲溴辛托品(1×10⁻⁶ - 3.2×10⁻⁴ M)可引起正性肌力反应,而辛巴生则不能。用利血平预处理动物可增强这些反应。利血平处理动物后的反应不受酚妥拉明(1×10⁻⁶ M)拮抗,但受普萘洛尔(1×10⁻⁶ M)拮抗。3. 甲溴辛托品而非辛巴生在心脏毒蕈碱受体上表现出变构抑制作用,导致Schild图呈曲线。在使用阿托品和甲溴辛托品的联合剂量比实验中也观察到偏离竞争性拮抗的情况。在1×10⁻⁶ M时,甲溴辛托品的pKB值为7.88±0.15(平均值±标准误,n = 5)。辛巴生在心脏毒蕈碱受体上的pA2值为8.52±0.06(n = 3)。4. 在气管和食管肌层黏膜平滑肌受体上,两种拮抗剂的Schild图均为线性。甲溴辛托品在这两种制剂受体上的pA2值相似(分别为6.08±0.05和6.03±0.09,n = 4),约比在心房受体上观察到的值低60倍。辛巴生在气管和食管肌层黏膜的毒蕈碱受体上也表现出相似的值(分别为7.61±0.05和7.57±0.04,n = 4)。5. 介导大鼠主动脉内皮舒张的毒蕈碱受体上,甲溴辛托品的pA2值(5.87±0.12,n = 6)与在平滑肌中观察到的相似,但与心房中的不同。辛巴生在内皮毒蕈碱受体上的pA2值比在平滑肌毒蕈碱受体上观察到的值低约0.5个pA2单位(6.92 + 0.80,n = 6)。此外,甲溴辛托品和辛巴生在这些受体上的Schild斜率显著(P < 0.05)小于1。6. 甲溴辛托品以及程度较轻的辛巴生是心脏毒蕈碱受体的强效和选择性拮抗剂。然而,鉴于该化合物的变构抑制特性和直接正性肌力作用,在解释甲溴辛托品的数据时应谨慎。
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