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印度贯叶连翘的脑内神经递质受体结合及益智研究

Brain neurotransmitter receptor binding and nootropic studies on Indian Hypericum perforatum Linn.

作者信息

Kumar Vikas, Khanna V K, Seth P K, Singh P N, Bhattacharya S K

机构信息

Department of Pharmaceutics, Institute of Technology, Banaras Hindu University, Varanasi, India.

出版信息

Phytother Res. 2002 May;16(3):210-6. doi: 10.1002/ptr.1101.

Abstract

The high affinity binding sites for serotonin and benzodiazepine in the frontal cortex, for dopamine in the striatum and muscarinic cholinergic receptors in the hippocampus were investigated in the brains of Charles Foster rats treated for 3 days. Transfer latency on elevated plus maze (TL), passive and active avoidance behaviour (PA and AA) and electroconvulsive shock (ECS) induced amnesia were also studied. Pilot studies indicated that single dose administration of Indian Hypericum perforatum (IHp) had little or no acute behavioural effects and hence the extract of IHp was administered orally at two dose levels (100 and 200 mg/kg, p.o.) once daily for 3 consecutive days, while piracetam (500 mg/kg, i.p.), a clinically used nootropic agent, was administered acutely to rats as the standard nootropic agent. Control rats were treated with an equal volume of vehicle (0.3% carboxymethyl cellulose). The results indicate that IHp treatment caused a significant decrease in the binding of [3H] spiroperone (DA-D2 receptor) to the striatum and an increase in the binding of [3H] ketanserin (5-HT2A receptor) and [3H] flunitrazepam (BDZ receptor) to the frontal cortex in rats. Preliminary pharmacological studies with IHp extract indicate the presence of two major behavioural actions, namely, antidepressant and anxiolytic. The present findings tend to elucidate the mechanism of earlier observations, the downregulation of the dopamine D2 receptor being consonant with anxiolytic and the upregulation of 5-HT2A and BDZ receptors being consonant with antidepressant activity. Piracetam when given alone, shortened the TL on days 1, 2 and 9 day and also antagonized the amnesic effects of ECS on the TL significantly, whereas IHp antagonized the amnesia produced by ECS. IHp had no significant effect per se on the retention of the PA in rats but produced a significant reversal of ECS induced PA retention deficit. Piracetam showed a significant facilitatory effect per se on PA retention and also reversed the ECS induced impaired PA retention. In the AA test, piracetam facilitated the acquisition and retention of AA in rats but IHp had no effect per se. Both the doses of IHp and piracetam significantly attenuated the ECS induced impaired retention of AA. These results indicate a possible nootropic action of IHp in amnesic animals, which was comparable qualitatively to piracetam.

摘要

在接受了3天治疗的查尔斯·福斯特大鼠的大脑中,研究了前额叶皮质中5-羟色胺和苯二氮卓的高亲和力结合位点、纹状体中多巴胺的高亲和力结合位点以及海马体中毒蕈碱胆碱能受体的高亲和力结合位点。还研究了高架十字迷宫上的转移潜伏期(TL)、被动和主动回避行为(PA和AA)以及电惊厥休克(ECS)诱导的失忆。初步研究表明,单剂量给予印度贯叶连翘(IHp)几乎没有或没有急性行为影响,因此,将IHp提取物以两种剂量水平(100和200mg/kg,口服)连续3天每天口服一次,而将临床上使用的促智药吡拉西坦(500mg/kg,腹腔注射)作为标准促智药急性给予大鼠。对照大鼠用等体积的赋形剂(0.3%羧甲基纤维素)治疗。结果表明,IHp治疗导致大鼠纹状体中[3H]螺哌隆(DA-D2受体)的结合显著减少,前额叶皮质中[3H]酮色林(5-HT2A受体)和[3H]氟硝西泮(BDZ受体)的结合增加。对IHp提取物的初步药理学研究表明存在两种主要的行为作用,即抗抑郁和抗焦虑。目前的研究结果倾向于阐明早期观察结果的机制,多巴胺D2受体的下调与抗焦虑一致,5-HT2A和BDZ受体的上调与抗抑郁活性一致。单独给予吡拉西坦可缩短第1、2和9天的TL,并且还显著拮抗ECS对TL的失忆作用,而IHp拮抗ECS产生的失忆。IHp本身对大鼠PA的保持没有显著影响,但可显著逆转ECS诱导的PA保持缺陷。吡拉西坦本身对PA保持有显著的促进作用,并且也逆转了ECS诱导的PA保持受损。在AA试验中,吡拉西坦促进大鼠AA的获得和保持,但IHp本身没有作用。IHp和吡拉西坦的两种剂量均显著减轻了ECS诱导的AA保持受损。这些结果表明IHp在失忆动物中可能具有促智作用,其在质量上与吡拉西坦相当。

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