首页> 外文期刊>European Journal of Pharmacology: An International Journal >Intrathecal co-administration of morphine and nimodipine produces higher antinociceptive effect by synergistic interaction as evident by injecting different doses of each drug in rats.
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Intrathecal co-administration of morphine and nimodipine produces higher antinociceptive effect by synergistic interaction as evident by injecting different doses of each drug in rats.

机译:鞘内共同施用吗啡和尼莫地平可通过协同相互作用产生更高的镇痛作用,如在大鼠中注射不同剂量的每种药物所证明的。

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摘要

Earlier, we reported that morphine-nimodipine combination produces significantly higher antinociception after intrathecal but not after systemic administration in mice. Different doses of morphine and nimodipine (5 microg of morphine, 5 microg of nimodipine, 5 microg each of morphine and nimodipine, 10 microg of morphine, 10 microg of nimodipine, 10 microg morphine with 5 microg nimodipine and 5 microg of morphine with 10 microg of nimodipine) were now injected intrathecally in Wistar rats to further characterise this antinociceptive effect. The acute antinociceptive effect was measured by the tail-flick test between 15 min to 7 h. The onset of maximum antinociception (100% MPE) was earlier (by 15 min) in nimodipine (5 microg) than in morphine (5 microg) treated group (by 30 min). Though earlier in onset, 5 microg nimodipine produced transient antinociception, which was significantly higher than saline treated controls for the initial 30 min only. Morphine (5 microg) produced significantly higher antinociception between 15 min to 3:30 h in comparison to control animals. However, co-administration of both morphine and nimodipine led to significantly higher antinociception than morphine alone at 4:00 h and also between 5:00 to 6:30 h. Interestingly, the combined antinociceptive action of morphine and nimodipine was not significantly different from 10 microg of morphine, which indicated synergistic interaction. Naloxone (5 mg/kg) could reverse this antinociceptive effect of morphine-nimodipine combination though it failed to reverse nimodipine (5 microg)-mediated antinociception at 15 min. Increasing the dose of either morphine or nimodipine to 10 mug did not increase antinociception except between 6:30-7:00 h. No obvious side effect was noted after administration of either morphine or nimodipine or both.
机译:早些时候,我们报道了吗啡-尼莫地平联合治疗在鞘内注射后可产生更高的抗伤害感受,但在小鼠全身给药后则不会。不同剂量的吗啡和尼莫地平(5微克吗啡,5微克尼莫地平,5微克吗啡和尼莫地平各,10微克吗啡,10微克尼莫地平,10微克吗啡和5微克尼莫地平以及5微克吗啡和10微克现在将鞘内注射尼莫地平(Nimdipine)的大鼠注射入Wistar大鼠,以进一步表征这种镇痛作用。在15分钟至7小时之间通过甩尾试验测量了急性镇痛作用。在尼莫地平(5微克)中最大抗伤害感受(100%MPE)的发作(在15分钟前)比吗啡(5微克)治疗组更早(在30分钟前)。尽管发病较早,但5微克尼莫地平产生短暂的抗伤害感,仅在最初的30分钟内显着高于盐水治疗的对照组。与对照动物相比,吗啡(5微克)在15分钟至3:30小时之间产生了更高的抗伤害感受。但是,吗啡和尼莫地平的共同给药在4:00 h以及5:00至6:30 h时比单独使用吗啡显着提高了抗伤害感受。有趣的是,吗啡和尼莫地平的联合镇痛作用与10微克吗啡没有显着差异,表明协同相互作用。纳洛酮(5 mg / kg)可以逆转吗啡-尼莫地平组合的镇痛作用,尽管它在15分钟时不能逆转尼莫地平(5微克)介导的镇痛作用。将吗啡或尼莫地平的剂量增加到10马克杯不会增加抗伤害感受,除非在6:30-7:00时之间。服用吗啡或尼莫地平或两者均未观察到明显的副作用。

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