Effects of chronic treatment with citalopram on cannabinoid and opioid receptor-mediated G-protein coupling in discrete rat brain regions.

Hesketh SA; Brennan AK; Jessop DS; Finn DP

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Effects of chronic treatment with citalopram on cannabinoid and opioid receptor-mediated G-protein coupling in discrete rat brain regions.

机译：西酞普兰慢性治疗对离散大鼠脑区域中大麻素和阿片受体介导的G蛋白偶联的影响。

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RATIONALE: There is growing interest in investigating the mechanisms of action of selective serotonin reuptake inhibitors (SSRIs), beyond their association with the serotonergic system, due to their wide therapeutic potential for disorders including depression, pain and addiction. OBJECTIVE: The aim of this study was to investigate whether chronic treatment with the SSRI, citalopram, alters the functional coupling of G(i/o)-associated cannabinoid type 1 (CB(1)) and mu-opioid receptors in selected areas of rat brain implicated in psychiatric disorders and pain. METHODS: Using an autoradiographic approach, the effects of the cannabinoid receptor agonist, HU210 (in the presence or absence of the CB(1) receptor antagonist AM251), or the mu-opioid receptor agonist, [D: -Ala(2),N-Me-Phe4,Gly(5)-ol]-enkephalin (DAMGO; in the presence or absence of the mu-opioid receptor antagonist D: -Phe-Cys-Tyr-D: -Trp-Orn-Thr-Pen-Thr-NH(2)), on [(35)S]GTPgammaS binding in discrete brain regions of citalopram-treated (10 mgkg(-1) day(-1) for 14 days by subcutaneous minipump) and control rats were investigated. RESULTS: The HU210-induced increase in [(35)S]GTPgammaS binding observed in the hypothalamic paraventricular nucleus of control rats was abolished after chronic treatment with citalopram. Reduced response to HU210 in rats receiving chronic treatment with citalopram was also observed in the hippocampus and medial geniculate nucleus. Citalopram had no significant effect on DAMGO-induced [(35)S]GTPgammaS binding in the brain regions investigated, with the exception of the medial geniculate nucleus where a modest impairment was observed. CONCLUSIONS: These data provide evidence for reduced cannabinoid receptor-mediated G-protein coupling in the hypothalamus, hippocampus and medial geniculate nucleus of rats chronically treated with citalopram, effects which may, in part, underlie the mechanism of action of SSRIs.

机译：理由：研究血清5-羟色胺再摄取抑制剂（SSRIs）与血清素能系统的联系之外，由于它们对包括抑郁症，疼痛和成瘾在内的疾病具有广泛的治疗潜力，因此越来越有兴趣研究其作用机制。目的：本研究的目的是调查用SSRI西酞普兰进行的慢性治疗是否会改变G（i / o）相关的1型大麻素（CB（1））和mu阿片受体在某些地区的功能偶联。大鼠大脑牵涉精神疾病和疼痛。方法：使用放射自显影方法，研究大麻素受体激动剂HU210（在存在或不存在CB（1）受体拮抗剂AM251的情况下）或μ阿片受体激动剂[D：-Ala（2）， N-Me-Phe4，Gly（5）-ol]-脑啡肽（DAMGO;在存在或不存在mu阿片受体拮抗剂D的情况下：-Phe-Cys-Tyr-D：-Trp-Orn-Thr-Pen- Thr-NH（2））对西酞普兰治疗的离散脑区（皮下微型泵10 mgkg（-1）day（-1）连续14天）的[（35）S] GTPgammaS结合进行了研究。结果：西酞普兰长期治疗后，消除了HU210诱导的在对照组大鼠下丘脑室旁核中[（35）S]GTPγS结合的增加。在海马和内侧膝状核中也观察到接受西酞普兰慢性治疗的大鼠对HU210的反应降低。西酞普兰对DAMGO诱导的[（35）S] GTPgammaS结合在被研究的大脑区域没有显着影响，除了内侧膝状核可见适度的损伤。结论：这些数据提供了证据证明，长期用西酞普兰治疗的大鼠下丘脑，海马和内侧膝状核中大麻素受体介导的G蛋白偶联减少，其作用可能部分是SSRI作用机理的基础。

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《Psychopharmacology》 |2008年第1期|共8页
作者
Hesketh SA; Brennan AK; Jessop DS; Finn DP;
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正文语种 eng
中图分类药学;
关键词
Citalopram; Chronic; therapeutic aspects; Brain; Receptors; Opioid; 西酞普兰; 脑; 受体; 阿片样;

机译：Citalopram;Chronic;therapeutic aspects;Brain;Receptors;Opioid;西酞普兰;脑;受体;阿片样;

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1. Effects of chronic treatment with citalopram on cannabinoid and opioid receptor-mediated G-protein coupling in discrete rat brain regions. [J] . Hesketh SA, Brennan AK, Jessop DS, Psychopharmacology . 2008,第1期

机译：西酞普兰慢性治疗对离散大鼠脑区域中大麻素和阿片受体介导的G蛋白偶联的影响。
2. Chronic ethanol consumption reduces delta-and mu-opioid receptor-stimulated G-protein coupling in rat brain. [J] . Saland LC, Abeyta A, Frausto S, Alcoholism: Clinical and experimental research . 2004,第1期

机译：慢性乙醇的消耗减少了大鼠大脑中δ和μ阿片受体刺激的G蛋白偶联。
3. Agonist treatment did not affect association of mu opioid receptors with lipid rafts and cholesterol reduction had opposite effects on the receptor-mediated signaling in rat brain and CHO cells. [J] . Huang P, Xu W, Yoon SI, Brain research . 2007,第0期

机译：激动剂治疗不影响μ阿片受体与脂筏的结合，胆固醇的降低对大鼠脑和CHO细胞中受体介导的信号传导具有相反的作用。
4. 5-HT_7 Receptor-Mediated Meningeal Dilatation Induced by 5-Carboxamidotryptamine in Rats is Not Altered by 5-HT Depletion and Chronic Corticosterone Treatment [C] . Martinez-Garcia E., Sanchez-Maldonado C. Terron J.A. Western Pharmacology Society . 2011

机译：5-HT_7受体介导的5-羧胺酰胺肽在大鼠中诱导的大鼠诱导的脑膜扩张不会通过5-HT耗尽和慢性皮质酮处理来改变
5. Effects of chronic administration of a D3 dopamine receptor preferring agonist on the Akt/GSK3/3 pathway in striatal brain regions. [D] . Prasad, Sheela. 2016

机译：长期给予首选D3多巴胺受体激动剂对纹状体脑区域Akt / GSK3 / 3途径的影响。
6. Agonist treatment did not affect association of mu opioid receptors with lipid rafts and cholesterol reduction had opposite effects on the receptor-mediated signaling in rat brain and CHO cells [O] . Peng Huang, Wei Xu, Su-In Yoon, -1

机译：激动剂治疗不会影响mu阿片受体与脂质筏的结合胆固醇的降低对大鼠脑和CHO细胞中受体介导的信号传导具有相反的作用
7. Agonist treatment did not affect association of mu opioid receptors with lipid rafts and cholesterol reduction had opposite effects on the receptor-mediated signaling in rat brain and CHO cells [O] . Peng Huang, Wei Xu, Su-In Yoon, 2007

机译：激动剂治疗不影响Mu阿片受体与脂质筏和胆固醇还原对大鼠脑和CHO细胞中受体介导的信号传导的影响

Effects of chronic treatment with citalopram on cannabinoid and opioid receptor-mediated G-protein coupling in discrete rat brain regions.

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