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神经节苷脂GM1可减轻东莨菪碱诱导的大鼠和小鼠失忆。

Ganglioside GM1 attenuates scopolamine-induced amnesia in rats and mice.

作者信息

Silva R H, Felicio L F, Frussa-Filho R

机构信息

Departamento de Farmacologia, Escola Paulista de Medicina, Universidade Federal de São Pualo, UNIFESP, SP, Brazil.

出版信息

Psychopharmacology (Berl). 1999 Jan;141(2):111-7. doi: 10.1007/s002130050814.

Abstract

Some experimental evidence suggests that the beneficial effects of monosialoganglioside GM1 on learning and memory could be related to an improving effect in central cholinergic function. The present study investigates the effects of GM1 on the memory impairment induced by scopolamine in rats or mice tested in passive (PA) and discriminative avoidance (DA) tasks, respectively. Wistar EPM-1 male rats and Swiss EPM-M1 male mice were treated daily IP with 50 mg/kg GM1 or saline for 7 or 14 days, respectively. Twenty-four hours after the last injection, GM1-treated animals received 1 mg/kg scopolamine (GM1-SCO) and saline-treated animals received 1 mg/kg scopolamine (SAL-SCO) or saline (SAL-SAL) IP. Twenty minutes later, the animals were submitted to PA or DA conditioning, and tests were performed 24 h later. The latency in entering the dark chamber of the PA apparatus (LD) presented by SAL-SCO rats was significantly decreased when compared to that presented by SAL-SAL animals. GM1-SCO animals showed an increased LD when compared to SAL-SCO animals and were not significantly different from SAL-SAL rats. GM1-SCO and SAL-SAL (but not SAL-SCO) mice spent significantly less time in the aversive enclosed arm of the discriminative avoidance apparatus when compared to the time spent in the non-aversive enclosed arm. The results are consistent with the interpretation that GM1 attenuates scopolamine-induced amnesia. Although not eliminating the participation of other transmitter systems, the present study indicates a possible role of central cholinergic transmission in the action of this compound on learning and memory.

摘要

一些实验证据表明,单唾液酸神经节苷脂GM1对学习和记忆的有益作用可能与改善中枢胆碱能功能有关。本研究分别考察了GM1对东莨菪碱诱导的大鼠或小鼠记忆损伤的影响,实验采用被动回避(PA)和辨别性回避(DA)任务。Wistar EPM-1雄性大鼠和瑞士EPM-M1雄性小鼠分别每天腹腔注射50 mg/kg GM1或生理盐水,持续7天或14天。末次注射24小时后,GM1处理组动物腹腔注射1 mg/kg东莨菪碱(GM1-SCO),生理盐水处理组动物腹腔注射1 mg/kg东莨菪碱(SAL-SCO)或生理盐水(SAL-SAL)。20分钟后,对动物进行PA或DA条件训练,并在24小时后进行测试。与SAL-SAL组动物相比,SAL-SCO组大鼠进入PA装置暗箱的潜伏期(LD)显著缩短。与SAL-SCO组动物相比,GM1-SCO组动物的LD延长,且与SAL-SAL组大鼠无显著差异。与在非厌恶封闭臂中花费的时间相比,GM1-SCO组和SAL-SAL组(而非SAL-SCO组)小鼠在辨别性回避装置的厌恶封闭臂中花费的时间显著减少。结果支持GM1可减轻东莨菪碱诱导的失忆这一解释。尽管本研究并未排除其他递质系统的参与,但表明中枢胆碱能传递在该化合物对学习和记忆的作用中可能发挥作用。

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