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牛虹膜括约肌、气管平滑肌和面部动脉中去甲肾上腺素的失活机制:对β-肾上腺素能受体介导反应的影响

Mechanisms of inactivation of noradrenaline in the iris sphincter, tracheal muscle and facial artery of cattle: implications for beta-adrenoceptor-mediated responses.

作者信息

Kalsner S

出版信息

Br J Pharmacol. 1978 Dec;64(4):545-52. doi: 10.1111/j.1476-5381.1978.tb17316.x.

Abstract

1 The role of neuronal and extraneuronal pathways of amine inactivation in regulating the inhibitory actions of noradrenaline was investigated in three bovine smooth muscle preparations in which the primary adrenoceptor is of the beta-type.2 The extraneuronal uptake inhibitor, 17beta-oestradiol, sensitized the inhibitory responses to noradrenaline in the facial artery, the iris sphincter and in tracheal muscle preparations, indicating a major role for non-neuronal processes in agonist-inactivation in all three preparations. Cocaine also increased responses to noradrenaline, pointing to a role for neuronal uptake either as a terminating mechanism or as a process limiting access of exogenous agonist molecules to their site of action.3 Cocaine did not enhance significantly responses to isoprenaline, a potent beta-adrenoceptor agonist which is not taken up neuronally. Further, relaxations to metaraminol, a sympathomimetic amine which is taken up extraneuronally, but much less so than noradrenaline, were also less enhanced by 17beta-oestradiol in the three preparations tested. These findings support the specificity of action of cocaine and 17beta-oestradiol as neuronal and extraneuronal uptake inhibitors in the present experiments.4 Studies of the uptake of [(3)H]-noradrenaline revealed that 17beta-oestradiol reduced the uptake of amine in the presence of cocaine, confirming a cocaine-resistant site of action for the steroid in all three preparations.5 It is concluded that extraneuronal uptake sites are located sufficiently close to the beta-adrenoceptors to modulate the concentration and duration of action of noradrenaline at these sites of action. It is proposed that in smooth muscles which contain a preponderance of beta-receptors, extraneuronal metabolism is a key event in terminating the inhibitory effects produced.

摘要
  1. 在三种以β型为主的肾上腺素能受体的牛平滑肌制剂中,研究了胺类失活的神经元和非神经元途径在调节去甲肾上腺素抑制作用中的作用。

  2. 非神经元摄取抑制剂17β - 雌二醇使面动脉、虹膜括约肌和气管肌肉制剂对去甲肾上腺素的抑制反应敏感化,表明在所有这三种制剂中,非神经元过程在激动剂失活中起主要作用。可卡因也增加了对去甲肾上腺素的反应,表明神经元摄取作为一种终止机制或作为限制外源性激动剂分子到达其作用部位的过程发挥作用。

  3. 可卡因对异丙肾上腺素(一种不被神经元摄取的强效β - 肾上腺素能激动剂)的反应没有显著增强。此外,在测试的三种制剂中,对间羟胺(一种非神经元摄取但比去甲肾上腺素摄取少得多的拟交感胺)的松弛作用也较少被17β - 雌二醇增强。这些发现支持了在本实验中可卡因和17β - 雌二醇作为神经元和非神经元摄取抑制剂的作用特异性。

  4. 对[³H] - 去甲肾上腺素摄取的研究表明,17β - 雌二醇在可卡因存在下减少了胺的摄取,证实了该类固醇在所有三种制剂中具有抗可卡因的作用位点。

  5. 结论是,非神经元摄取位点位于足够接近β - 肾上腺素能受体的位置,以调节去甲肾上腺素在这些作用位点的浓度和作用持续时间。有人提出,在含有大量β受体的平滑肌中,非神经元代谢是终止所产生抑制作用的关键事件。

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