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初级传入神经元在炎症皮肤中表达功能性δ阿片受体。

Primary afferent neurons express functional delta opioid receptors in inflamed skin.

作者信息

Brederson Jill-Desiree, Honda Christopher N

机构信息

Department of Pharmacology, University of Minnesota, Minneapolis, MN 55455, USA.

Department of Neuroscience, University of Minnesota, Minneapolis, MN 55455, USA.

出版信息

Brain Res. 2015 Jul 21;1614:105-11. doi: 10.1016/j.brainres.2015.04.023. Epub 2015 Apr 22.

Abstract

Peripherally-restricted opiate compounds attenuate hyperalgesia in experimental models of inflammatory pain, but have little discernable effect on nociceptive behavior in normal animals. This suggests that activation of opioid receptors on peripheral sensory axons contributes to decreased afferent activity after injury. Previously, we reported that direct application of morphine to cutaneous receptive fields decreased mechanical and heat-evoked responses in a population of C-fiber nociceptors in inflamed skin. Consistent with reported behavioral studies, direct application of morphine had no effect on fiber activity in control skin. The aim of the present study was to determine whether mechanical responsiveness of nociceptors innervating inflamed skin was attenuated by direct activation of delta opioid receptors (DORs) on peripheral terminals. An ex vivo preparation of rat plantar skin and tibial nerve was used to examine effects of a selective DOR agonist, deltorphin II, on responsiveness of single fibers innervating inflamed skin. Electrical recordings were made eighteen hours after injection of complete Freund's adjuvant into the hindpaw. Deltorphin II produced an inhibition of the mechanical responsiveness of single fibers innervating inflamed skin; an effect blocked by the DOR-selective antagonist, naltrindole. The population of units responsive to deltorphin II was identified as consisting of C fiber mechanical nociceptors.

摘要

外周限制性阿片类化合物可减轻炎症性疼痛实验模型中的痛觉过敏,但对正常动物的伤害性感受行为几乎没有明显影响。这表明外周感觉轴突上阿片受体的激活有助于损伤后传入活动的减少。此前,我们报道过将吗啡直接应用于皮肤感受野可降低炎症皮肤中一群C纤维伤害感受器的机械和热诱发反应。与已报道的行为学研究一致,将吗啡直接应用于对照皮肤对纤维活动没有影响。本研究的目的是确定通过直接激活外周终末上的δ阿片受体(DORs)是否能减弱支配炎症皮肤的伤害感受器的机械反应性。采用大鼠足底皮肤和胫神经的离体标本,研究选择性DOR激动剂二丙诺啡对支配炎症皮肤的单根纤维反应性的影响。在将完全弗氏佐剂注射到后爪18小时后进行电记录。二丙诺啡可抑制支配炎症皮肤的单根纤维的机械反应性;该效应被DOR选择性拮抗剂纳曲吲哚阻断。对二丙诺啡有反应的神经元群体被确定为由C纤维机械伤害感受器组成。

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