血管扩张性香兰素型β受体阻滞剂的脂溶性对β-肾上腺素受体亚型的功能和结合活性的影响

Bin-Nan Wu, Kuo-Pyng Shen, Rong-Jyh Lin, Yeun-Chih Huang, Lien-Chai Chiang, Yi-Ching Lo, Chiu-Yin Lin, Ing-Jun Chen
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引用次数: 5

摘要

在豚鼠右心房、气管和大鼠结肠上研究了各种香草型β-肾上腺素受体阻滞剂的作用。此外,我们还研究了它们的β1-, β2-和β3-肾上腺素受体结合亲和力。所有这些β-肾上腺素能拮抗剂以浓度依赖性的方式抑制(−)异丙肾上腺素诱导的右心房和气管舒张反应的正变时效应。其中一些药物可以防止(−)异丙肾上腺素对大鼠结肠自发运动的抑制。在测试的药物中,我们发现阿魏地洛尔、丁香地洛尔、丁香地洛尔、异丁香地洛尔和阿魏地洛尔,以及心得安尔和美托洛尔,具有β3-肾上腺素受体阻断活性,其他药物几乎没有效果。此外,我们在[3H]CGP-12177 (β1/β2-肾上腺素受体阻滞剂和β3-肾上腺素受体激动剂)中评估了香草素型β-肾上腺素能拮抗剂的结合特性,它们分别与大鼠脑室、肺和肩关节间棕色脂肪组织(IBAT)膜中的β1-、β2-和β3-肾上腺素受体位点结合。丁香酚、丁香酚、美托洛尔、异丁香酚和阿魏酚在竞争β3-肾上腺素受体结合位点时的效力低于心得安和阿魏酚。从体外功能和结合研究的结果来看,我们认为心得安、阿魏地洛尔、丁香地洛尔、丁香地洛尔、美托洛尔、异丁香地洛尔和阿魏地洛尔都具有阻断β3-肾上腺素受体的活性。另一方面,我们还发现丁香酚、丁香酚、美托洛尔、异丁香酚和阿魏酚与心得安和阿魏酚相比具有较低的脂溶性。综上所述,我们认为这些香草素型β受体阻滞剂的β3-肾上腺素受体拮抗作用与其脂溶性呈正相关。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Lipid solubility of vasodilatory vanilloid-type β-blockers on the functional and binding activities of β-adrenoceptor subtypes

Various vanilloid-type β-adrenoceptor blockers were studied on guinea pig right atrium and trachea and rat colon. In addition, we also investigated their β1-, β2-, and β3-adrenoceptor binding affinities. All these β-adrenergic antagonists inhibited (−)isoproterenol-induced positive chronotropic effects of the right atrium and tracheal relaxation responses in a concentration-dependent manner. Some of these agents prevented the inhibition of rat colon spontaneous motility by (−)isoproterenol. Of the agents tested, we found that ferulidilol, eugenodilol, eugenolol, isoeugenolol, and ferulinolol, as well as propranolol and metoprolol, possessed β3-adrenoceptor blocking activities, others were nearly without effectiveness. Furthermore, the binding characteristics of vanilloid-type β-adrenergic antagonists were evaluated in [3H]CGP-12177, a β12-adrenoceptor blocker and a β3-adrenoceptor agonist, binding to β1-, β2-, and β3-adrenoceptor sites in rat ventricle, lung, and interscapular brown adipose tissue (IBAT) membranes, respectively. Eugenodilol, eugenolol, metoprolol, isoeugenolol, and ferulinolol were less potent than both propranolol and ferulidilol in competing for the β3-adrenoceptor binding sites. From the results of in vitro functional and binding studies, we suggested that propranolol, ferulidilol, eugenodilol, eugenolol, metoprolol, isoeugenolol, and ferulinolol all possessed β3-adrenoceptor blocking activities. On the other hand, we also found that eugenodilol, eugenolol, metoprolol, isoeugenolol, and ferulinolol had a low lipid solubility in comparison with propranolol and ferulidilol. In conclusion, we proposed that β3-adrenoceptor antagonistic actions of these vanilloid-type β-blockers were positively correlated with their lipid solubility.

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