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Involvement of cholinergic receptors in the different stages of memory measured in the modified elevated plus maze test in mice

机译:在改良的高架迷宫试验中测得胆碱能受体参与不同阶段的记忆

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Background and Methods: Several lines of evidence support a strong relationship between cholinergic pathways and memory. The aim of our experiments was to examine the mechanisms involved in the formation of different memory stages, to evaluate the impact of substances, which affect the cholinergic system in mice, with an employment of the modified elevated plus maze (mEPM) test. This test allows examining different processes of memory (acquisition, consolidation and retrieval), depending on the time of drug treatment. The time period, necessary for mice to move from the opened arm to the enclosed arm (i.e., transfer latency, TL) was used as an index of memory. Results: Our findings revealed that in both memory acquisition and consolidation, nicotine, an agonist of cholinergic receptors (0.035 and 0.175 mg/kg, free base, sc), reduced TL on the second day of the experiment (TL2), thus improving memory. In turn, scopolamine, an antagonist of cholinergic receptors (0.3 and 1.0 mg/kg, ip), significantly increased TL2 values, impairing cognition. Subsequently, we evaluated the influence of mecamylamine, a non-selective antagonist of nicotinic cholinergic receptors (nAChRs) and of varenicline, an α4β2 partial nAChRs agonist, on memory-related behaviors induced by nicotine and scopolamine. Acute injections of mecamylamine (0.5 and 1.0 mg/kg, ip) and varenicline (0.5 and 1.0 mg/kg, ip), prior to the injections of nicotine (0.035 mg/kg) or scopolamine (1.0 mg/kg), significantly suppressed nicotine-induced memory improvement or scopolamine-induced memory impairment. Conclusion: Our studies indicate that the cholinergic system plays a crucial role in memory processes. Pharmacological manipulation of cholinergic transmission can be the base to develop more effective pharmacotherapies for these memory disturbances in which cholinergic receptors are involved.
机译:背景与方法:几条证据支持胆碱能途径与记忆之间的密切关系。我们的实验目的是通过使用改良的高架迷宫(mEPM)测试来检查参与不同记忆阶段形成的机制,以评估影响小鼠胆碱能系统的物质的影响。该测试允许根据药物治疗的时间来检查不同的记忆过程(获取,合并和检索)。小鼠从张开的手臂移动到封闭的手臂所需的时间段(即,传输等待时间,TL)被用作记忆的指标。结果:我们的发现表明,在记忆获得和巩固中,胆碱能受体激动剂尼古丁(0.035和0.175 mg / kg,游离碱,皮下注射)在实验的第二天(TL2)降低了TL,从而改善了记忆。反过来,胆碱能受体的拮抗剂东0.3碱(0.3和1.0 mg / kg,腹膜内)显着增加TL2值,损害认知。随后,我们评估了烟碱胆碱能受体(nAChRs)的非选择性拮抗药美甲胺和α4β2部分nAChRs激动剂伐尼克兰对尼古丁和东pol碱诱导的记忆相关行为的影响。注射尼古丁(0.035 mg / kg)或东pol碱(1.0 mg / kg)之前,急性注射美加明胺(0.5和1.0 mg / kg,腹腔内)和缬尼克兰(0.5和1.0 mg / kg,腹膜内)尼古丁引起的记忆改善或东pol碱引起的记忆障碍。结论:我们的研究表明胆碱能系统在记忆过程中起着至关重要的作用。胆碱能传递的药理学操纵可以成为开发针对这些涉及胆碱能受体的记忆障碍的更有效药物疗法的基础。

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