首页> 外文期刊>European Journal of Pharmacology: An International Journal >Differential effects of systemic and intraseptal administration of the acetylcholinesterase inhibitor tacrine on the recovery of spatial behavior in an animal model of diencephalic amnesia.
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Differential effects of systemic and intraseptal administration of the acetylcholinesterase inhibitor tacrine on the recovery of spatial behavior in an animal model of diencephalic amnesia.

机译:全身和隔壁给予乙酰胆碱酯酶抑制剂他克林对双脑性失忆动物模型中空间行为恢复的不同作用。

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Several lines of evidence suggest that acetylcholinesterase inhibitors (AChE) have their cognitive enhancing effects by stimulating cholinergic receptors within the medial septum. However, intraseptal administration of cholinergic enhancing drugs produce mixed results that appear to depend on both the integrity of the medial septum as well as task demands. Three experiments were conducted to determine the relationship between increased cholinergic activity within the medial septum and hippocampus and behavioral recovery in a model of diencephalic amnesia produced by pyrithiamine-induced thiamine deficiency (PTD). In Experiment 1, systemic tacrine (0.0, 0.75, 1.5mg/kg) was administered to PTD and pair-fed (PF) rats prior to a spontaneous alternation task. Without tacrine, PF rats alternated at a higher rate than PTD rats. Both doses of tacrine increased alternation in PTD rats to within the range of PF rats. In Experiment 2, three doses of intraseptal tacrine (2.5, 5.0, 12.5microg) were administered to PTD and PF rats and changes in hippocampal acetylcholine efflux were assessed. Both the 5.0 and 12.5microg doses significantly increased hippocampal acetylcholine levels, but the change was greater in the PTD rats. In Experiment 3, despite the fact that both intraseptal doses of tacrine (5.0, 12.5microg) increased hippocampal acetylcholine levels, only 5.0microg significantly improved alternation scores in PTD rats. Thus, when there is basal forebrain cholinergic cell loss in conjunction with diencephalic pathology, the therapeutic range of AChE-I in the medial septum and the effective doses do not directly map onto changes in acetylcholine efflux in the hippocampus.
机译:有几条证据表明,乙酰胆碱酯酶抑制剂(AChE)通过刺激内侧间隔内的胆碱能受体而具有认知增强作用。然而,胆碱能增强药物的隔室给药产生混合结果,这似乎取决于内侧隔的完整性以及任务要求。进行了三个实验,以确定在由巯乙胺诱发的硫胺素缺乏症(PTD)产生的双脑性失忆症模型中,中隔和海马内胆碱能活性增加与行为恢复之间的关系。在实验1中,在自发轮换任务之前,先对PTD和成对喂养(PF)的大鼠给药全身性他克林(0.0、0.75、1.5mg / kg)。没有他克林,PF大鼠的交替率要高于PTD大鼠。两种剂量的他克林都使PTD大鼠的交替增加到PF大鼠的范围内。在实验2中,对PTD和PF大鼠给予三剂量的隔中他克林(2.5、5.0、12.5microg),并评估海马乙酰胆碱外流的变化。 5.0和12.5微克剂量均显着增加海马乙酰胆碱水平,但在PTD大鼠中变化更大。在实验3中,尽管事实上隔室注射两次他克林剂量(5.0,12.5microg)都会增加海马的乙酰胆碱水平,但只有5.0microg显着改善了PTD大鼠的交替评分。因此,当基础脑前胆碱能细胞损失与双脑病相结合时,内侧隔中AChE-1的治疗范围和有效剂量不能直接映射到海马体乙酰胆碱外排的变化。

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