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胆囊收缩素B受体激动剂BC264腹腔注射大鼠后可增加伏隔核中的多巴胺水平,并促进动机和注意力。

The CCK-B agonist, BC264, increases dopamine in the nucleus accumbens and facilitates motivation and attention after intraperitoneal injection in rats.

作者信息

Ladurelle N, Keller G, Blommaert A, Roques B P, Daugé V

机构信息

Département de Pharmacochimie Moléculaire et Structurale, U 266 INSERM, URA D 1500 CNRS, Faculté des Sciences Pharmaceutiques et Biologiques, Paris, France.

出版信息

Eur J Neurosci. 1997 Sep;9(9):1804-14. doi: 10.1111/j.1460-9568.1997.tb00747.x.

DOI:10.1111/j.1460-9568.1997.tb00747.x
PMID:9383203
Abstract

Although it is known that panic attacks are triggered by the cholecystokinin fragment CCK4, the specific involvement of peripheral or central cholecystokinin CCK receptors in various adaptive processes such as emotion, memory and anxiety has yet to be demonstrated. With this aim, we have investigated the biochemical and pharmacological effects resulting from the administration of BC264, a highly potent and selective CCK-B agonist able to cross the blood-brain barrier. Very low doses of BC264 (microg/kg i.p.), increased the exploration of animals submitted to an unknown territory but were devoid of anxiogenic properties in the elevated plus maze. BC264 increased locomotion and rearings of rats newly placed in an open field and improved their spontaneous alternation in a Y-maze. The use of vagotomized animals showed that the increased alternation induced by BC264 did not require an intact vagus nerve, unlike the locomotor activation. These behavioural effects, prevented by the prior i.p. administration of the CCK-B antagonist L-365,260 but not by the CCK-A antagonist L-364,718, were shown to depend on dopaminergic systems, since they were blocked by D1 (SCH23390, 25 microg/kg i.p.) or D2 (sulpiride, 50 or 100 mg/kg i.p.) antagonists. In addition, bilateral perfusion in freely moving rats of BC264 at pharmacologically active doses, using a newly designed microdialysis system, was found to increase the extracellular levels of DA, DOPAC and HVA in the anterior part of the nucleus accumbens. These results show that activation of CCK-B receptors by BC264 does not produce anxiogenic-like effects but appears to improve motivation and attention, whereas other CCK-B agonists such as BocCCK4 induce anxiogenic responses. Several explanations, including the existence of different sub-sites of the CCK-B receptor, could account for these differential effects.

摘要

尽管已知惊恐发作是由胆囊收缩素片段CCK4触发的,但外周或中枢胆囊收缩素CCK受体在诸如情绪、记忆和焦虑等各种适应性过程中的具体参与情况尚未得到证实。出于这个目的,我们研究了BC264给药所产生的生化和药理作用,BC264是一种能够穿过血脑屏障的高效且选择性的CCK - B激动剂。极低剂量的BC264(微克/千克腹腔注射)增加了处于未知区域的动物的探索行为,但在高架十字迷宫中没有致焦虑特性。BC264增加了新放置在旷场中的大鼠的运动和竖毛行为,并改善了它们在Y迷宫中的自发交替行为。使用迷走神经切断的动物表明,与运动激活不同,BC264诱导的交替行为增加不需要完整的迷走神经。这些行为效应在预先腹腔注射CCK - B拮抗剂L - 365,260后被阻断,但在注射CCK - A拮抗剂L - 364,718后未被阻断,结果表明它们依赖于多巴胺能系统,因为它们被D1(SCH23390,25微克/千克腹腔注射)或D2(舒必利,50或100毫克/千克腹腔注射)拮抗剂阻断。此外,使用新设计的微透析系统对自由活动的大鼠双侧灌注药理活性剂量的BC264,发现可增加伏隔核前部细胞外多巴胺、3,4 - 二羟基苯乙酸和高香草酸的水平。这些结果表明,BC264激活CCK - B受体不会产生类焦虑效应,但似乎能改善动机和注意力,而其他CCK - B激动剂如BocCCK4则会诱导焦虑反应。包括CCK - B受体存在不同亚位点在内的几种解释可以说明这些差异效应。

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