尼可地尔对神经性疼痛和伤害性疼痛的抗伤害感受作用部分通过TRPV1/阿片类信号传导介导。
The Antinociceptive Effect of Nicorandil in Neuropathic and Nociceptive Pain is Partially Mediated via TRPV1/Opioidergic Signaling.
作者信息
Badr Rasha M, Abuiessa Salwa A, Elblehi Samar S, Hassan Nayera W, Afify Elham A
机构信息
Department of Pharmacology and Toxicology, Faculty of Pharmacy, University of Alexandria, 1-El-Khartoum Square, Azarita, Alexandria, Postal Code: 21521, Egypt.
Department of Pathology, Faculty of Veterinary Medicine, University of Alexandria, Alexandria, Egypt.
出版信息
Mol Neurobiol. 2025 Jun 20. doi: 10.1007/s12035-025-05136-5.
Neuropathic pain is a serious neurological disorder caused by lesioned somatosensory neurons characterized by multiple pathologies. Transient receptor potential vanilloid 1 (TRPV1) channels and opioid receptors are co-expressed in dorsal root ganglia (DRG) and play a crucial role in the development of neuropathic pain. Here, we investigated the possible involvement of TRPV1 channels and µ-opioid receptors in mediating the antinociception of the K opener, nicorandil, in neuropathic pain in four nociceptive models: chronic constriction injury of the sciatic nerve (CCI), formalin, capsaicin, and acetic acid writhing tests. Nicorandil (150 mg/kg, twice, 2 h apart, PO) administered to male rats (i) reversed the effects of CCI on nociceptive threshold and cumulative scores assessed by von Frey and acetone test, respectively; (ii) reduced licking time and number of flinches in biphasic formalin and capsaicin tests, and (iii) reduced the number of writhes in the acetic acid test; and (iv) combined nicorandil-capsaicin abolished acetic acid induced writhing response. Similarly, ipsilateral intraplantar injection of nicorandil (37.5 mg/paw, twice, ipl) inhibited nociceptive responses induced by capsaicin, formalin, and acetic acid. Immunohistochemical analysis revealed that nicorandil blunted the CCI-induced elevation of TRPV1 protein expression in DRG. The beneficial effects of nicorandil in all models were attenuated by naloxone. Molecular docking supported the interaction between nicorandil and TRPV1. Histologically, nicorandil improved the pathological changes induced by CCI in the sciatic nerve and DRG. Collectively, these results demonstrate that nicorandil exhibits antinociceptive effects in neuropathic and nociceptive pain via mechanisms involving TRPV1 modulation and opioid receptor signaling. Further investigation is warranted to explore the mechanism of action of nicorandil as an alternative treatment option for neuropathic pain.
神经病理性疼痛是一种由受损的体感神经元引起的严重神经障碍,具有多种病理特征。瞬时受体电位香草酸亚型1(TRPV1)通道和阿片受体在背根神经节(DRG)中共同表达,并在神经病理性疼痛的发生发展中起关键作用。在此,我们在四种伤害性模型中研究了TRPV1通道和μ-阿片受体在介导钾通道开放剂尼可地尔对神经病理性疼痛的镇痛作用中的可能参与情况:坐骨神经慢性缩窄损伤(CCI)、福尔马林、辣椒素和醋酸扭体试验。给雄性大鼠口服尼可地尔(150 mg/kg,分两次给药,间隔2小时):(i)分别逆转了CCI对通过von Frey和丙酮试验评估的伤害性阈值和累积评分的影响;(ii)在双相福尔马林和辣椒素试验中减少了舔舐时间和退缩次数,(iii)在醋酸试验中减少了扭体次数;(iv)尼可地尔与辣椒素联合使用消除了醋酸诱导的扭体反应。同样,同侧足底注射尼可地尔(37.5 mg/爪,分两次注射)抑制了辣椒素、福尔马林和醋酸诱导的伤害性反应。免疫组织化学分析显示,尼可地尔减弱了CCI诱导的DRG中TRPV1蛋白表达的升高。纳洛酮减弱了尼可地尔在所有模型中的有益作用。分子对接支持了尼可地尔与TRPV1之间的相互作用。组织学上,尼可地尔改善了CCI在坐骨神经和DRG中诱导的病理变化。总的来说,这些结果表明,尼可地尔通过涉及TRPV1调节和阿片受体信号传导的机制,在神经病理性疼痛和伤害性疼痛中表现出镇痛作用。有必要进一步研究以探索尼可地尔作为神经病理性疼痛替代治疗选择的作用机制。
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