曲马多的镇痛作用不受阿片类受体介导的小鼠术后立即疼痛

Angela Maria Sousa, Hazem Adel Ashmawi
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引用次数: 1

摘要

背景与目的司马多是一种中枢镇痛药,用于治疗中度至重度疼痛。局部镇痛作用已被证明,部分原因是局部麻醉样作用,但其他机制尚不清楚。外周阿片受体在局部镇痛作用中的作用尚不清楚。在本研究中,我们在足底切口模型中检测了外周阿片受体在曲马多局部镇痛作用中的作用。方法年轻雄性Wistar大鼠分为7组:对照组、曲马多足底注射组、曲马多足底注射组、纳洛酮-曲马多足底注射组、纳洛酮-曲马多足底注射组、纳洛酮-曲马多足底注射组、纳洛酮-曲马多足底注射组、纳洛酮-曲马多足底静脉注射组、纳洛酮静脉注射组。给药(曲马多5 mg、纳洛酮200 μg或0.9% NaCl)后,将大鼠进行足底切开,分别于切开后基线、10、15、30、45和60 min评估von Frey纤维机械刺激后的戒断阈值。结果对照组足底切口在整个观察期间均出现明显的机械性痛觉过敏,足底曲马多组、足底纳洛酮-足底曲马多组和静脉纳洛酮-足底曲马多组均未出现机械性痛觉过敏。曲马多静脉组的停药阈值晚于45min后升高,纳洛酮-曲马多静脉组和纳洛酮静脉组在整个过程中均保持痛觉过敏。结论司马多具有减轻足底切口机械性痛觉的早期局部镇痛作用。这种镇痛作用不是由外周阿片受体介导的。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
El efecto analgésico del tramadol no está mediado por receptores opiáceos en el dolor en ratones en el postoperatorio inmediato

Background and objectives

Tramadol is known as a central acting analgesic drug, used for the treatment of moderate to severe pain. Local analgesic effect has been demonstrated, in part due to local anesthetic-like effect, but other mechanisms remain unclear. The role of peripheral opioid receptors in the local analgesic effect is not known. In this study, we examined role of peripheral opioid receptors in the local analgesic effect of tramadol in the plantar incision model.

Methods

Young male Wistar rats were divided into seven groups: control, intraplantar tramadol, intravenous tramadol, intravenous naloxone-intraplantar tramadol, intraplantar naloxone-intraplantar tramadol, intravenous naloxone-intravenous tramadol, and intravenous naloxone. After receiving the assigned drugs (tramadol 5 mg, naloxone 200 μg or 0.9% NaCl), rats were submitted to plantar incision, and withdrawal thresholds after mechanical stimuli with von Frey filaments were assessed at baseline, 10, 15, 30, 45 and 60 min after incision.

Results

Plantar incision led to marked mechanical hyperalgesia during the whole period of observation in the control group, no mechanical hyperalgesia were observed in intraplantar tramadol group, intraplantar naloxone-intraplantar tramadol group and intravenous naloxone-intraplantar tramadol. In the intravenous tramadol group a late increase in withdrawal thresholds (after 45 min) was observed, the intravenous naloxone-intravenous tramadol group and intravenous naloxone remained hyperalgesic during the whole period.

Conclusions

Tramadol presented an early local analgesic effect decreasing mechanical hyperalgesia induced by plantar incision. This analgesic effect was not mediated by peripheral opioid receptors.

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