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神经活动对猫尾状核中由L-[3H]色氨酸持续生成的[3H]5-羟色胺体内释放的影响。

Effect of nerve activity on the in vivo release of [3H]serotonin continuously formed from L-[3H]tryptophan in the caudate nucleus of the cat.

作者信息

Héry F, Simonnet G, Bourgoin S, Soubrié P, Artaud F, Hamon M, Glowinski J

出版信息

Brain Res. 1979 Jun 22;169(2):317-34. doi: 10.1016/0006-8993(79)91033-3.

Abstract

A new isotopic approach has been developed to study the in vivo release of serotonin (5-HT). 'Encéphale isolé' cats were implanted with a push-pull cannula in the ventrocaudal part of the head of the caudate nucleus to estimate the release of [3H]5-HT continuously synthesized from L-[3H]tryptophan. Both [3H]5-HT and [3H]tryptamine were found in superfusates. Resting steady state in the release of [3H]indoleamines was observed as soon as 20 min after the beginning of the superfusion with L-[3H]tryptophan; the levels of [3H]5-HT in superfusates were 2.5 times those of [3H]tryptamine and about 6 times the blank value. They were markedly enhanced in the presence of fluoxetine (5 x 10(-6)M), a blocker of the 5-HT uptake process. A marked increase in the release of [3H]5-HT was seen during the local depolarization of 5-HT terminals with potassium chloride (60 mM) or batrachotoxin (10(-6)M) or during the stimulation of 5-HT cell bodies in the nucleus raphe dorsalis with L-glutamic acid (5 x 10(-5)M). These treatments did not enhance the efflux of [3H]tryptamine. The potassium-evoked release of [3H]5-HT was reduced by LSD (10(-5)M). LSD added alone in the superfusing fluid was without effect. The batrachotoxin-evoked release of [3H]5-HT was inhibited in the presence of tetrodotoxin (9 x 10(-6)M). The spontaneous release of [3H]5-HT and [3H]tryptamine was markedly reduced in the presence of a calcium-free medium containing cobalt (10 mM). A transient slight reduction in the spontaneous release of [3H]5-HT was observed in the presence of tetrodotoxin (9 x 10(-6)M). The local cooling of 5-HT cell bodies with a cryoelectrode induced a slight reversible decrease in [3H]5-HT release. These last two treatments were without significant effect on [3H]tryptamine efflux in superfusates. These results indicate that the release of [3H]5-HT endogenously formed from [3H]tryptophan is dependent on nerve activity and that this is not the case for [3H]tryptamine. The advantages of the isotopic approach for in vivo studies on the release of 5-HT are discussed.

摘要

已开发出一种新的同位素方法来研究5-羟色胺(5-HT)的体内释放。将“孤立脑”猫在尾状核头部腹尾部分植入推挽式套管,以估计由L-[3H]色氨酸连续合成的[3H]5-HT的释放。在灌流液中发现了[3H]5-HT和[3H]色胺。在用L-[3H]色氨酸开始灌流后20分钟,就观察到了[3H]吲哚胺释放的静息稳态;灌流液中[3H]5-HT的水平是[3H]色胺的2.5倍,约为空白值的6倍。在5-HT摄取过程的阻断剂氟西汀(5×10(-6)M)存在的情况下,它们显著增加。在用氯化钾(60 mM)或蛙毒素(10(-6)M)使5-HT终末局部去极化期间,或在用L-谷氨酸(5×10(-5)M)刺激中缝背核中的5-HT细胞体期间,观察到[3H]5-HT的释放显著增加。这些处理并未增强[3H]色胺的流出。LSD(10(-5)M)使钾诱发的[3H]5-HT释放减少。单独添加到灌流液中的LSD没有作用。在河豚毒素(9×10(-6)M)存在的情况下,蛙毒素诱发的[3H]5-HT释放受到抑制。在含有钴(10 mM)的无钙培养基中,[3H]5-HT和[3H]色胺的自发释放显著减少。在河豚毒素(9×10(-6)M)存在的情况下,观察到[3H]5-HT的自发释放有短暂的轻微减少。用冷冻电极对5-HT细胞体进行局部冷却,导致[3H]5-HT释放有轻微的可逆性减少。最后这两种处理对灌流液中[3H]色胺的流出没有显著影响。这些结果表明,由[3H]色氨酸内源性形成的[3H]5-HT的释放依赖于神经活动,而[3H]色胺则不然。讨论了同位素方法在5-HT释放的体内研究中的优点。

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