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Both neuronal and non-neuronal acetylcholine take part in non-quantal acetylcholine release in the rat atrium.

机译:神经元和非神经元的乙酰胆碱都参与大鼠心房中非定量的乙酰胆碱释放。

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摘要

In mammalian myocardium acetylcholine (ACh), neurotransmitter which strikingly affects the cardiomyocytes, can be released from the neurons both via quantal (vesicular) and nonquantal (non-vesicular) mechanism of secretion. Non-quantal release is continuous, independent on vagus activity and provides accumulation of ACh in myocardium in the presence of acetylcholinesterase (AChE) inhibitors. The aim of the present study was to determine the source of non-quantal ACh in isolated atrial myocardium of adult and newborn rats.Standard microelectrode technique was used to determine the cholinergic changes of electrical activity under the action of AChE inhibitor paraoxon, which correlates with the intensity of nonquantal ACh release.In adult rats selective inhibitor of neuronal choline uptake system hemicholinium III (10(-5) M) decreased all effects of paraoxon (5 × 10(-6) M) more than twofold. Inhibitor of polyspecific 3 organic cation transporters corticosterone (10(-4) M) also significantly decreased effects of paraoxon in adult rats, indicating that non-neuronal ACh, which is synthesized by cardiomyocytes, takes part in accumulation of ACh in the myocardium. When hemicholinium III and corticosterone were applied together, paraoxon effects in adult atrial myocardium were suppressed almost completely. In newborn rats cardiomyocytes do not excrete ACh. In accordance with this fact hemicholinium III completely abolished effects of paraoxon in newborn myocardium, while corticosterone was ineffective. Thus, non-quantal ACh is released both from cholinergic nerves and cardiomyocytes in adult rat myocardium, while it has exclusively neuronal nature in newborns.The study demonstrates dual neuronal and non-neuronal nature of non-quantal ACh in the heart.
机译:在哺乳动物的心肌乙酰胆碱(ACh)中,可显着影响心肌细胞的神经递质可以通过定量(囊泡)和非定量(非囊泡)分泌机制从神经元中释放出来。非定量释放是连续的,独立于迷走神经活动,并在乙酰胆碱酯酶(AChE)抑制剂存在下提供ACh在心肌中的蓄积。本研究的目的是确定成年和新生大鼠离体心房心肌中非定量ACh的来源。采用标准微电极技术测定在AChE抑制剂对氧磷作用下胆碱能的电活动变化,这与在成年大鼠中,神经元胆碱摄取系统hemicholiniumium III(10(-5)M)的选择性抑制剂使对氧磷(5×10(-6)M)的所有作用降低两倍以上。多特异性3型有机阳离子转运蛋白皮质酮(10(-4)M)的抑制剂也显着降低了对氧磷对成年大鼠的影响,表明心肌细胞合成的非神经元ACh参与了心肌中ACh的积累。当hemicholinium III和皮质酮一起使用时,对成人心房心肌的对氧磷作用几乎被完全抑制。在新生大鼠中,心肌细胞不分泌ACh。根据这一事实,hemicholinium III完全消除了对氧磷对新生心肌的作用,而皮质酮无效。因此,成年大鼠心肌非胆碱能乙酰胆碱能从胆碱能神经和心肌细胞中释放出来,而在新生儿中则具有非神经元本质。这项研究证明了心脏非胆碱能乙酰胆碱具有神经元和非神经元双重性质。

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