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胆囊收缩素 - 多巴胺共存:与胆囊收缩素受体亚型相对应的电生理作用。

Cholecystokinin-dopamine coexistence: electrophysiological actions corresponding to cholecystokinin receptor subtype.

作者信息

Hommer D W, Stoner G, Crawley J N, Paul S M, Skirboll L R

出版信息

J Neurosci. 1986 Oct;6(10):3039-43. doi: 10.1523/JNEUROSCI.06-10-03039.1986.

Abstract

Cholecystokinin (CCK)-like peptides when administered intravenously produce 2 distinct actions on the single-unit activity of mesencephalic dopamine (DA) neurons in the rat: an excitatory action and a potentiation of the inhibitory effects of DA agonists. The ability of several CCK fragments that have been shown to bind selectively to the peripheral and/or the central CCK-binding sites were examined for their ability to induce either excitation or a potentiation of DA. Only sulfated CCK-8 was able to induce excitation of mesencephalic DA neurons, but both sulfated and unsulfated CCK-8, as well as CCK-4, potentiated the inhibitory effects of the DA agonist apomorphine (APO). CCK-3 failed to potentiate APO-induced inhibition. Both of these effects appeared to be confined to cell bodies in regions of the ventral tegmental area and substantia nigra, zona compacta that have been reported to contain both DA and CCK. Thus, CCK-like peptides that have been shown to bind to the high-affinity CCK binding site in brain potentiated the effects of DA. In contrast, the ability of CCK-like peptides to induce neuronal excitation corresponds with their affinity for the peripheral-type CCK binding site.

摘要

静脉注射胆囊收缩素(CCK)样肽对大鼠中脑多巴胺(DA)神经元的单单位活动产生两种不同作用:兴奋作用和增强DA激动剂的抑制作用。研究了几种已被证明能选择性结合外周和/或中枢CCK结合位点的CCK片段诱导DA兴奋或增强作用的能力。只有硫酸化CCK-8能够诱导中脑DA神经元兴奋,但硫酸化和未硫酸化的CCK-8以及CCK-4均能增强DA激动剂阿扑吗啡(APO)的抑制作用。CCK-3未能增强APO诱导的抑制作用。这两种作用似乎都局限于腹侧被盖区和黑质致密部区域的细胞体,据报道这些区域同时含有DA和CCK。因此,已被证明能与脑中高亲和力CCK结合位点结合的CCK样肽增强了DA的作用。相比之下,CCK样肽诱导神经元兴奋的能力与其对外周型CCK结合位点的亲和力相对应。

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Receptor selectivity of cholecystokinin effects on mesoaccumbens dopamine neurons.
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