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神经元摄取抑制剂、尼索西汀和氟西汀对大鼠血管收缩的影响。

Neuronal uptake inhibitors, nisoxetine and fluoxetine on rat vascular contractions.

作者信息

Cohen M L, Wiley K S

出版信息

Eur J Pharmacol. 1977 Aug 1;44(3):219-29. doi: 10.1016/0014-2999(77)90069-3.

Abstract

The importance of neuronal uptake processes in rat arteries and veins was compared using nisoxetine and fluoxetine, selective inhibitors for neuronal uptake of norepinephrine and serotonin, respectively. Nisoxetine (10(-7) - 10(-5) M) increased the sensitivity to exogenous norepinephrine in the portal and mesenteric veins (10-fold) and in the mesenteric artery (2.5-fold). Responses to field stimulation were also increased afternisoxetine in all three vessels. After nisoxetine, aortic responses to norepinephrine were unaltered and in all tissues, serotonin-induced contractions were reduced. Fluoxetine did not potentiate responses to norepinephrine or to field stimulation except in the mesenteric vein where sensitivity to norepinephrine was increased and the relaxation rate after field stimulation was prolonged. Although serotonin has been detected in blood vessels, fluoxetine did not increase vascular responses to serotonin. These studies suggest that rat mesenteric veins have a highly sensitive neuronal uptake mechanism of norepinephrine. Furthermore, these data provide indirect evidence against a functionally important serotonergic uptake process in rat blood vessels and suggest that neuronal uptake of serotonin does not exert a major role in terminating the vascular action of this biogenic amine.

摘要

分别使用去甲肾上腺素和5-羟色胺神经元摄取的选择性抑制剂尼索西汀和氟西汀,比较大鼠动脉和静脉中神经元摄取过程的重要性。尼索西汀(10⁻⁷ - 10⁻⁵M)增加了门静脉和肠系膜静脉对外源性去甲肾上腺素的敏感性(10倍)以及肠系膜动脉的敏感性(2.5倍)。在所有三种血管中,尼索西汀处理后对场刺激的反应也增强。尼索西汀处理后,主动脉对去甲肾上腺素的反应未改变,并且在所有组织中,5-羟色胺诱导的收缩均减弱。氟西汀除了在肠系膜静脉中增加了对去甲肾上腺素的敏感性并延长了场刺激后的舒张速率外,并未增强对去甲肾上腺素或场刺激的反应。尽管在血管中已检测到5-羟色胺,但氟西汀并未增加血管对5-羟色胺的反应。这些研究表明,大鼠肠系膜静脉具有高度敏感的去甲肾上腺素神经元摄取机制。此外,这些数据提供了间接证据,反对大鼠血管中功能上重要的5-羟色胺能摄取过程,并表明5-羟色胺的神经元摄取在终止这种生物胺的血管作用中不发挥主要作用。

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