maarein -2抑制炎性和神经性三叉神经节疼痛,减少三叉神经节的神经元激活

Raphael Vieira Lopes , Darciane Favero Baggio , Camila Rodrigues Ferraz , Mariana Marques Bertozzi , Telma Saraiva-Santos , Waldiceu Aparecido Verri Junior , Juliana Geremias Chichorro
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引用次数: 1

摘要

疼痛是与涉及口面部结构的疾病相关的常见症状。大多数急性口面部疼痛很容易识别,但药物治疗可能受到当前可用药物的不良事件和/或患者特征的限制。此外,慢性口面部疼痛在诊断和治疗方面都是临床挑战。越来越多的证据表明,专门的促溶解脂质介质(SPMs)除了在解决炎症方面具有良好的作用外,还具有有效的镇痛作用。maaresin (MaR-1和MaR-2)是该家族中最后被描述的成员,MaR-2的镇痛作用尚未报道。本文研究了MaR-2在不同口腔面部疼痛模型中的作用。MaR-2(1或10 ng)总是通过髓质蛛网膜下注射给药,这与鞘内治疗相对应。单次注射MaR-2可显著降低大鼠口腔面部福尔马林试验的I期和II期。在大鼠术后疼痛模型中,反复注射MaR-2可防止面部发热和机械性痛觉过敏的发生。在三叉神经性疼痛(CCI-ION)模型中,反复注射MaR-2可逆转大鼠和小鼠的面部热和机械性痛觉过敏。CCI-ION增加三叉神经节(TG) c-Fos阳性神经元和CGRP+激活(核pNFkB)神经元,经MaR-2重复处理后恢复到假手术水平。综上所述,MaR-2对口面部源性炎症性和神经性疼痛具有有效且持久的镇痛作用,TG中cgrp阳性神经元的抑制可能是MaR-2作用的原因。
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Maresin-2 inhibits inflammatory and neuropathic trigeminal pain and reduces neuronal activation in the trigeminal ganglion

Pain is a common symptom associated with disorders involving the orofacial structures. Most acute orofacial painful conditions are easily recognized, but the pharmacological treatment may be limited by the adverse events of current available drugs and/or patients’ characteristics. In addition, chronic orofacial pain conditions represent clinical challenges both, in terms of diagnostic and treatment. There is growing evidence that specialized pro-resolution lipid mediators (SPMs) present potent analgesic effects, in addition to their well characterized role in the resolution of inflammation. Maresins (MaR-1 and MaR-2) were the last described members of this family, and MaR-2 analgesic action has not yet been reported. Herein the effect of MaR-2 in different orofacial pain models was investigated. MaR-2 (1 or 10 ng) was always delivered via medullary subarachnoid injection, which corresponds to the intrathecal treatment. A single injection of MaR-2 caused a significant reduction of phases I and II of the orofacial formalin test in rats. Repeated injections of MaR-2 prevented the development of facial heat and mechanical hyperalgesia in a model of post-operative pain in rats. In a model of trigeminal neuropathic pain (CCI-ION), repeated MaR-2 injections reversed facial heat and mechanical hyperalgesia in rats and mice. CCI-ION increased c-Fos positive neurons and CGRP+ activated (nuclear pNFkB) neurons in the trigeminal ganglion (TG), which were restored to sham levels by MaR-2 repeated treatment. In conclusion, MaR-2 showed potent and long-lasting analgesic effects in inflammatory and neuropathic pain of orofacial origin and the inhibition of CGRP-positive neurons in the TG may account for MaR-2 action.

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