首页> 外文期刊>Neuroscience: An International Journal under the Editorial Direction of IBRO >Antinociceptive effects of choline against acute and inflammatory pain.
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Antinociceptive effects of choline against acute and inflammatory pain.

机译:胆碱对急性和炎性疼痛的镇痛作用。

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We used the hot plate test and the formalin test to evaluate the antinociception of choline after i.c.v. or i.v. administration. The analgesic mechanism of choline was also studied. The response latency of mice was significantly prolonged in the hot plate test after choline (90-120 mug/animals) i.c.v. administration in a dose-dependent manner. Pretreatment with methyllycaconitine citrate (MLA), alpha-bungarotoxin, or atropine blocked the antinociception of choline in the hot plate test. In contrast, mecamylamine and naloxone had no effect. No antinociceptive action of choline was found in the hot plate test, but it did have an effect in the late phase of the formalin test after i.v. administration. The effect of choline on anti-inflammatory pain was blocked by MLA, but not by mecamylamine, naloxone and atropine, which is indicative of the involvement of alpha7 receptors in peripheral sites. When choline (2 mg/kg) was coadministered with aspirin (9.4 mg/kg), the licking/biting times in the late phase significantly decreased, although no effects were shown when these doses of drugs were used alone. Similarly, coadministration of choline (2 mg/kg) with morphine (0.165 mg/kg) significantly increased the antinociception of morphine in the late phase, but had no effect in the early phase. These results demonstrate that activation of alpha7 nicotinic receptors by choline elicits antinociceptive effects both in an acute thermal pain model and in an inflammatory pain model. Choline holds promise for development as a non-addictive analgesic drug and in reducing the regular dose of aspirin or morphine in inflammatory pain.
机译:我们使用热板试验和福尔马林试验评估了静脉内注射后胆碱的抗伤害感受。或i.v.行政。还研究了胆碱的镇痛作用。胆碱(90-120杯/动物)静脉注射后,在热板测试中小鼠的反应潜伏期显着延长。以剂量依赖性方式给药。在热板测试中,使用柠檬酸甲基卡卡尼碱(MLA),α-邦加罗毒素或阿托品进行预处理可阻止胆碱的抗伤害感受。相反,美卡明胺和纳洛酮没有作用。在热板试验中未发现胆碱的抗伤害感受作用,但在静脉注射后福尔马林试验的后期确实有作用。行政。胆碱对抗炎性疼痛的作用被MLA阻断,但未被美卡明,纳洛酮和阿托品阻断,这表明α7受体参与了外周部位。当胆碱(2 mg / kg)与阿司匹林(9.4 mg / kg)并用时,晚期的舔/咬时间显着减少,尽管单独使用这些剂量的药物未见效果。同样,胆碱(2 mg / kg)与吗啡(0.165 mg / kg)的共同给药在晚期显着增加了吗啡的抗伤害感受,但在早期没有作用。这些结果表明,在急性热痛模型和炎性痛模型中,胆碱对α7烟碱受体的激活均引起抗伤害作用。胆碱有望成为一种非成瘾性镇痛药,并有望减轻炎症性疼痛中阿司匹林或吗啡的常规剂量。

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