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神经刺激频率对灌注猫脾脏释放的3H-去甲肾上腺素代谢的影响:刺激期间及刺激后观察到的差异。

Influence of the frequency of nerve stimulation on the metabolism of 3H-norepinephrine released from the perfused cat spleen: differences observed during and after the period of stimulation.

作者信息

Dubocovich M L, Langer S Z

出版信息

J Pharmacol Exp Ther. 1976 Jul;198(1):83-101.

PMID:933013
Abstract

The metabolism of 3H-norepinephrine (3H-NE) released by different frequencies of nerve stimulation was studied in the perfused cat spleen after labeling the endogenous stores with (-)-3H-NE. For a wide range of frequencies of stimulation, unmetabolized 3H-NE represented between 50 and 60% of the total increase in outflow of radioactivity elicited by nerve stimulation. The deaminated glycol, 3,4-dihydroxyphenylglycol (3H-DOPEG), was the main metabolite of 3H-NE released by nerve stimulation. When the increase in outflow of radioactivity was analyzed for the samples collected during nerve stimulation, there was a progressive decrease in the fraction of 3H-NE released which was collected as 3H-metabolites as the frequency of stimulation was increased from 0.5 to 5 Hz. For the samples collected in the poststimulation period, there was no frequency dependence in the metabolism of the released transmitter: approximately 75% of the total overflow of radioactivity was accounted for by the 3H-NE metabolites, particularly 3H-DOPEG. The time course of the metabolism of 3H-NE released by nerve stimulation revealed that 3H-DOPEG formation was rather small during stimulation and that it increased sharply in the poststimulation samples. The selective increase in 3H-DOPEG formation in the poststimulation period is compatible with the view that neuronal uptake of the released transmitter might be increased immediately after nerve stimulation. Inhibition of neuronal uptake by cocaine or by phenoxybenzamine prevented 3H-DOPEG formation from 3H-NE released by nerve stimulation. Yet, in the presence of cocaine, the fractional release of total radioactivity per shock was not increased at either 1, 5 or 30 Hz. These results support the view that a large fraction of the 3H-NE released by stimulation which is recaptured by nerve endings is metabolized to 3H-DOPEG rather than stored for subsequent reuse. The extensive conversion to 3H-DOPEG of 3H-NE released by nerve stimulation suggests that there may be a difference between the process of neuronal uptake under resting conditions and that which operates under conditions of nerve stimulation. This difference may be related to the concentration of the transmitter achieved in the synaptic gap in each experimental condition. Under resting conditions and during perfusion with low concentrations of NE, neuronal uptake in the perfused cat spleen is coupled with vesicular storage. On the other hand, when the extracellular concentration of NE is increased as a result of nerve stimulation, neuronal uptake of NE appears to be coupled with presynaptic metabolism through monoamine oxidase and aldehyde reductase.

摘要

在用(-)-3H-去甲肾上腺素标记内源性储存后,研究了灌注猫脾脏中不同频率神经刺激释放的3H-去甲肾上腺素(3H-NE)的代谢情况。在很宽的刺激频率范围内,未代谢的3H-NE占神经刺激引起的放射性流出总量增加的50%至60%。脱氨基二醇3,4-二羟基苯乙二醇(3H-DOPEG)是神经刺激释放的3H-NE的主要代谢产物。当分析神经刺激期间收集的样本的放射性流出增加情况时,随着刺激频率从0.5Hz增加到5Hz,以3H-代谢产物形式收集的释放的3H-NE的比例逐渐降低。对于刺激后阶段收集的样本,释放的递质的代谢不存在频率依赖性:放射性总溢出量的约75%由3H-NE代谢产物,特别是3H-DOPEG所致。神经刺激释放的3H-NE的代谢时间进程表明,刺激期间3H-DOPEG的形成相当少,而在刺激后样本中其急剧增加。刺激后阶段3H-DOPEG形成的选择性增加与神经刺激后神经元对释放的递质的摄取可能立即增加的观点一致。可卡因或苯氧苄胺对神经元摄取的抑制阻止了神经刺激释放的3H-NE形成3H-DOPEG。然而,在存在可卡因的情况下,每一次电击时总放射性的分数释放量在1Hz、5Hz或30Hz时均未增加。这些结果支持这样一种观点,即刺激释放的大部分3H-NE被神经末梢重新摄取后被代谢为3H-DOPEG,而不是储存以供后续再利用。神经刺激释放的3H-NE广泛转化为3H-DOPEG表明,静息条件下的神经元摄取过程与神经刺激条件下的神经元摄取过程可能存在差异。这种差异可能与每种实验条件下突触间隙中递质达到的浓度有关。在静息条件下以及用低浓度NE灌注期间,灌注猫脾脏中的神经元摄取与囊泡储存相关。另一方面,当由于神经刺激而使NE的细胞外浓度增加时,NE的神经元摄取似乎通过单胺氧化酶和醛还原酶与突触前代谢相关。

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