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腹腔注射生理盐水可调节海马脑受体复合物水平,但不损害 Morris 水迷宫中的表现。

Intraperitoneal injection of saline modulates hippocampal brain receptor complex levels but does not impair performance in the Morris Water Maze.

机构信息

Department of Pediatrics, Medical University of Vienna, Währinger Gürtel 18, 1090 Vienna, Austria.

出版信息

Amino Acids. 2012 Aug;43(2):783-92. doi: 10.1007/s00726-011-1130-9. Epub 2011 Nov 2.

Abstract

The involvement of the hippocampus in pain has been demonstrated but key players, i.e. the major brain receptors have not been shown to be modulated by pain. It was therefore the aim of the study to show the concerted action and pattern of brain receptor complex levels in a non-invasive model of moderate pain. C57BL/6J mice were divided into four groups of 14 animals each: trained injected, trained non-injected, yoked injected and yoked non-injected. Animals were tested in the open field and the elevated plus maze for behavioural evaluation and cognitive functions were tested using the Morris Water Maze. Hippocampi were taken 6 h following sacrification. Membrane proteins were prepared by ultracentrifugation and run on blue native gels to keep the native state, blotted to membranes and western blotting was carried out using the primary antibodies against serotonin receptor 5HT1A, muscarinic acetylcholine receptor M1 (mAChR-M1), nicotinic acetylcholine receptor alpha7 (nAChR-alpha7), glutamate (AMPA) receptor (GluR1) and neurokinin receptor 1 (NK-1). There was no difference between performance in behaviour or in the MWM between groups. Brain receptor level changes involved all receptors given above. Pain affected mAChR-M1, GluR1 and NK-1 complex levels when yoked-injected were compared with yoked non-injected animals. Memory mechanisms affected mAChR-M1 complex levels when trained non-injected animals were compared with yoked non-injected controls. Taken together, the neurochemical basis for testing receptor agonists/antagonists on the role of pain and the hippocampus was generated that may be useful for interpretations of the role of this complex area in moderate pain.

摘要

海马体在疼痛中的作用已得到证实,但关键的参与者,即主要的大脑受体,并没有被证明受到疼痛的调节。因此,本研究的目的是在一个非侵入性的中度疼痛模型中展示大脑受体复合物水平的协同作用和模式。C57BL/6J 小鼠分为四组,每组 14 只:训练注射组、训练未注射组、配对注射组和配对未注射组。动物在旷场和高架十字迷宫中进行行为评估,使用 Morris 水迷宫测试认知功能。牺牲后 6 小时取出海马体。通过超速离心制备膜蛋白,并在蓝色 native 凝胶上运行以保持天然状态,印迹到膜上,然后使用针对血清素受体 5HT1A、毒蕈碱乙酰胆碱受体 M1(mAChR-M1)、烟碱型乙酰胆碱受体α7(nAChR-α7)、谷氨酸(AMPA)受体(GluR1)和神经激肽受体 1(NK-1)的初级抗体进行 Western blot 分析。各组之间的行为或 MWM 表现没有差异。大脑受体水平的变化涉及上述所有受体。当与配对未注射的动物相比,配对注射的动物的 mAChR-M1、GluR1 和 NK-1 复合物水平受到疼痛的影响。当与配对未注射的对照组相比,训练未注射的动物的记忆机制影响 mAChR-M1 复合物水平。综上所述,本研究为测试受体激动剂/拮抗剂在疼痛和海马体中的作用提供了神经化学基础,这可能有助于解释该复杂区域在中度疼痛中的作用。

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