丁螺环酮对人类志愿者热感觉和痛阈的影响。

Goran Pavlaković, Julija Tigges, Thomas A Crozier
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引用次数: 26

摘要

背景:丁螺环酮是部分5-HT1A受体激动剂。动物研究表明,调节5-HT1A受体的5-羟色胺能传递可以诱导急性疼痛模型的镇痛。然而,到目前为止,还没有关于血清素受体激动剂对人类疼痛感知的影响的研究发表。方法:采用前瞻性、随机、双盲、双假、安慰剂对照研究,观察丁螺环酮(30 mg p.o)对12名女性志愿者(26±2岁)热感觉和疼痛阈值的影响,吗啡(10 mg静脉注射)为阳性对照。结果:吗啡在60分钟显著提高热痛检测阈值(DeltaT:安慰剂1.0℃和1.3℃,p < 0.05)。丁螺环酮在60分钟内对6名参与者产生轻度镇静作用,但对任何测量参数都没有影响。结论:丁螺环酮在最大推荐剂量下对热痛无显著影响。然而,由于它只是5-HT1A受体的部分激动剂,并且还作用于其他受体类型,因此本研究的阴性结果并不排除更特异性的5-HT1A受体激动剂可能具有镇痛作用。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Effect of buspirone on thermal sensory and pain thresholds in human volunteers.

Effect of buspirone on thermal sensory and pain thresholds in human volunteers.

Effect of buspirone on thermal sensory and pain thresholds in human volunteers.

Effect of buspirone on thermal sensory and pain thresholds in human volunteers.

Background: Buspirone is a partial 5-HT1A receptor agonist. Animal studies have shown that modulation of serotoninergic transmission at the 5-HT1A receptor can induce analgesia in acute pain models. However, no studies have been published so far on the effects of serotonin receptor agonists on pain perception in humans.

Methods: The effects of buspirone (30 mg p.o.) on thermal sensory and pain thresholds were investigated in twelve female volunteers (26 +/- 2 yrs) in a prospective, randomized, double-blind, double-dummy, placebo-controlled study with morphine (10 mg i.v.) as positive control.

Results: Morphine significantly increased the heat pain detection threshold (DeltaT: placebo 1.0 degrees C and 1.3 degrees C, p < 0.05) at 60 minutes. Buspirone caused mild sedation in six participants at 60 minutes, but was without effect on any of the measured parameters.

Conclusion: Buspirone in the maximal recommended dose was without significant effect on thermal pain. However, as it is only a partial agonist at the 5-HT1A receptor and also acts on other receptor types, the negative results of the present study do not rule out a possible analgesic effect of more specific 5-HT1A receptor agonists.

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