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首页> 外文期刊>Neurotoxicity research >Phencyclidine and Scopolamine for Modeling Amnesia in Rodents: Direct Comparison with the Use of Barnes Maze Test and Contextual Fear Conditioning Test in Mice
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Phencyclidine and Scopolamine for Modeling Amnesia in Rodents: Direct Comparison with the Use of Barnes Maze Test and Contextual Fear Conditioning Test in Mice

机译:用于啮齿动物的静脉内菊属植物的Phenyclidine和CoLopolamine:直接比较小鼠的Barnes迷宫试验和上下文恐惧调理试验

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Nowadays cognitive impairments are a growing unresolved medical issue which may accompany many diseases and therapies, furthermore, numerous researchers investigate various neurobiological aspects of human memory to find possible ways to improve it. Until any other method is discovered, in vivo studies remain the only available tool for memory evaluation. At first, researchers need to choose a model of amnesia which may strongly influence observed results. Thereby a deeper insight into a model itself may increase the quality and reliability of results. The most common method to impair memory in rodents is the pretreatment with drugs that disrupt learning and memory. Taking this into consideration, we compared the activity of agents commonly used for this purpose. We investigated effects of phencyclidine (PCP), a non-competitive NMDA receptor antagonist, and scopolamine (SCOP), an antagonist of muscarinic receptors, on short-term spatial memory and classical fear conditioning in mice. PCP (3mg/kg) and SCOP (1 mg/kg) were administrated intraperitoneally 30min before behavioral paradigms. To assess the influence of PCP and SCOP on short-term spatial memory, the Barnes maze test in C57BL/J6 mice was used. Effects on classical conditioning were evaluated using contextual fear conditioning test. Additionally, spontaneous locomotor activity of mice was measured. These two tests were performed in CD-1 mice. Our study reports that both tested agents disturbed short-term spatial memory in the Barnes maze test, however, SCOP revealed a higher activity. Surprisingly, learning in contextual fear conditioning test was impaired only by SCOP.
机译:如今的认知障碍是一种不断增长的未解决的医学问题,此外,许多疾病和疗法可能伴随着许多研究人员调查人类记忆的各种神经生物学方面,以找到改善它的可能方法。在发现任何其他方法之前,体内研究仍然是存储器评估的唯一可用工具。首先,研究人员需要选择一个可能强烈影响观察结果的艾尼西亚模型。从而深入了解模型本身可能会增加结果的质量和可靠性。在啮齿动物中损害记忆的最常见方法是扰乱学习和记忆的药物的预处理。考虑到这一点,我们比较了常用于此目的的代理活动。我们调查了Phenyclidine(PCP),非竞争性NMDA受体拮抗剂和CoCopolamine(SCOP),肌肉蛋白受体的拮抗剂,对小鼠的短期空间记忆和古典恐惧调理的影响。在行为范例之前,PCP(3mg / kg)和scop(1 mg / kg)腹腔内腹膜内施用30分钟。为了评估PCP和SCOP对短期空间记忆的影响,使用了C57BL / J6小鼠的Barnes迷宫测试。使用上下文恐惧调理试验评估对古典调理的影响。另外,测量小鼠的自发运动活性。这两个测试是在CD-1小鼠中进行的。我们的研究报告称,Barnes迷宫试验中的两种测试代理都扰乱了短期空间记忆,然而,SCOP揭示了更高的活动。令人惊讶的是,在语境恐惧调理测试中学习仅受SCOP损害。

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