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AMPA/海人藻酸拮抗剂LY293558可减轻辣椒素诱发的痛觉过敏,但对正常皮肤的疼痛无效。

AMPA/kainate antagonist LY293558 reduces capsaicin-evoked hyperalgesia but not pain in normal skin in humans.

作者信息

Sang C N, Hostetter M P, Gracely R H, Chappell A S, Schoepp D D, Lee G, Whitcup S, Caruso R, Max M B

机构信息

NIDR/NIH Pain Research Clinic, Pain and Neurosensory Mechanisms Branch, National Institute of Dental Research, National Institutes of Health, Bethesda, Maryland, USA.

出版信息

Anesthesiology. 1998 Nov;89(5):1060-7. doi: 10.1097/00000542-199811000-00005.

Abstract

BACKGROUND

Animal studies suggest that alpha-amino-3-hydroxy-5-methyl-4-isoxazole propionic acid-kainate (AMPA-KA) receptors are involved in pain processing. The effects of the competitive AMPA-KA antagonist LY293558 in two types of experimental pain in human volunteers, brief pain sensations in normal skin, and mechanical allodynia-pinprick hyperalgesia were studied after the injection of intradermal capsaicin.

METHODS

Brief intravenous infusions of the competitive AMPA-KA antagonist LY293558 were given to 25 healthy volunteers to examine acute toxicity and analgesic effects. Fifteen volunteers then entered a double-blinded, three-period crossover study. In a Phase II study, LY293558 infusions (100% maximally tolerated dose vs. 33% maximally tolerated dose vs. placebo) began 10 min after intradermal injection of 250 microg capsaicin in volar forearm. Spontaneous pain, areas of mechanical allodynia and pinprick hyperalgesia, and side effects were determined every 5 min for 60 min.

RESULTS

The median maximally tolerated dose was 1.3 +/- 0.4 (range, 0.9-2.0) mg/kg. Tests of cognitive and neurological function were unchanged. Dose-limiting side effects were hazy vision in 95% of volunteers and sedation in 40%. There were no significant changes in electrical or warm-cool detection and pain thresholds or heat pain thresholds. LY293558 had little effect on brief pain sensations in normal skin. Both high and low doses of LY293558 significantly reduced pain intensity, pain unpleasantness, and the area in which light brush evoked pain after intradermal capsaicin. There was a trend toward a dose-response effect of LY293558 on the area in which pinprick evoked pain after intradermal capsaicin, which did not reach statistical significance.

CONCLUSIONS

The authors infer that AMPA-KA receptor blockade reduces the spinal neuron sensitization that mediates capsaicin-evoked pain and allodynia. The low incidence of side effects at effective doses of LY293558 suggests that this class of drugs may prove to be useful in clinical pain states.

摘要

背景

动物研究表明,α-氨基-3-羟基-5-甲基-4-异恶唑丙酸-海人藻酸(AMPA-KA)受体参与疼痛处理。在皮内注射辣椒素后,研究了竞争性AMPA-KA拮抗剂LY293558对人类志愿者两种类型实验性疼痛、正常皮肤短暂疼痛感觉以及机械性异常性疼痛-针刺性痛觉过敏的影响。

方法

对25名健康志愿者进行竞争性AMPA-KA拮抗剂LY293558的短暂静脉输注,以检查急性毒性和镇痛效果。然后15名志愿者进入双盲、三阶段交叉研究。在一项II期研究中,在掌侧前臂皮内注射250微克辣椒素10分钟后开始LY293558输注(100%最大耐受剂量对比33%最大耐受剂量对比安慰剂)。每5分钟测定一次自发痛、机械性异常性疼痛和针刺性痛觉过敏区域以及副作用,共测定60分钟。

结果

最大耐受剂量中位数为1.3±0.4(范围0.9 - 2.0)毫克/千克。认知和神经功能测试无变化。剂量限制性副作用为95%的志愿者出现视物模糊,40%的志愿者出现镇静。电刺激或温冷觉检测及疼痛阈值或热痛阈值无显著变化。LY293558对正常皮肤短暂疼痛感觉影响不大。高剂量和低剂量的LY293558均显著降低皮内注射辣椒素后的疼痛强度、疼痛不适感以及轻刷诱发疼痛的区域。LY293558对皮内注射辣椒素后针刺诱发疼痛区域有剂量反应效应趋势,但未达到统计学显著性。

结论

作者推断,AMPA-KA受体阻断可降低介导辣椒素诱发疼痛和异常性疼痛的脊髓神经元致敏。LY293558有效剂量下副作用发生率低表明这类药物可能在临床疼痛状态中有用。

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