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柠檬酸镁可提高痛阈并降低大脑中 TLR4 浓度。

Magnesium Citrate Increases Pain Threshold and Reduces TLR4 Concentration in the Brain.

机构信息

Department of Physiology, School of Medicine, Dokuz Eylül University, Izmir, Turkey.

College of Vocational School of Health Services, School of Medicine, Dokuz Eylül University, Izmir, Turkey.

出版信息

Biol Trace Elem Res. 2021 May;199(5):1954-1966. doi: 10.1007/s12011-020-02384-5. Epub 2020 Sep 28.

DOI:10.1007/s12011-020-02384-5
PMID:32989649
Abstract

Magnesium is being investigated in various clinical conditions and has shown to be effective in some chronic pain models. However, it is not clear if oral magnesium use affects pain perception in acute pain. TLR4's (toll-like receptor) role in pain perception has emerged through its role in immune pathways and ion channels. The aim of this study is to investigate the effect of a single oral dose of magnesium citrate on pain conduction and whether with magnesium, the expression of TLR4 changes in the acute phase. Following a single dose of 66-mg/kg magnesium citrate administration to male Balb-c mice, pain perception (via hot-plate test), motor conduction (via electrophysiological recording, forelimb grip strength, rotarod and open-field tests), and emotional state (via elevated plus maze and forced swim test) were evaluated. In behavioral experiments, the control group was compared with applied magnesium for three different time groups (4, 8, 24 h). TLR4 expression was measured in four groups: control, magnesium (Mg), hot plate (HP), and Mg + HP. Hot plate latency was prolonged in the magnesium group (p < 0.0001) and electrophysiological recordings (p < 0.001) and forelimb grip strength measurement (p < 0.001) determined motor latency. Compared with the untreated hot plate group, TLR4 levels was lower in the brain (p = 0.023) and higher in the sciatic nerve (p = 0.001) in the magnesium-treated hot plate group. Consequently, the study indicated a single dose of magnesium citrate appeared to cause weakening in the transmission and perception of nociceptive pain. TLR4 may act as a regulator in magnesium's effects on pain perception.

摘要

镁正在各种临床情况下进行研究,并已证明在某些慢性疼痛模型中有效。然而,目前尚不清楚口服镁是否会影响急性疼痛的疼痛感知。TLR4( toll-like receptor )在疼痛感知中的作用已经通过其在免疫途径和离子通道中的作用而显现出来。本研究旨在研究柠檬酸镁单次口服剂量对疼痛传导的影响,以及镁是否会改变急性相 TLR4 的表达。在对雄性 Balb-c 小鼠单次给予 66-mg/kg 柠檬酸镁后,评估了疼痛感知(通过热板试验)、运动传导(通过电生理记录、前肢握力、转棒和旷场试验)和情绪状态(通过高架十字迷宫和强迫游泳试验)。在行为实验中,将对照组与应用镁的三个不同时间组(4、8、24 h)进行比较。在四组中测量 TLR4 表达:对照组、镁(Mg)、热板(HP)和 Mg+HP。镁组热板潜伏期延长(p < 0.0001),电生理记录(p < 0.001)和前肢握力测量(p < 0.001)确定运动潜伏期。与未经处理的热板组相比,镁处理的热板组中大脑中的 TLR4 水平较低(p = 0.023),而坐骨神经中的 TLR4 水平较高(p = 0.001)。因此,该研究表明柠檬酸镁单次剂量似乎会导致伤害性疼痛的传导和感知减弱。TLR4 可能在镁对疼痛感知的作用中起调节作用。

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The Chronic Use of Magnesium Decreases VEGF Levels in the Uterine Tissue in Rats.
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Nutrients. 2022 Apr 29;14(9):1863. doi: 10.3390/nu14091863.
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