高频电刺激可减轻神经元释放炎症介质，改善神经性疼痛。

Bioelectronic medicine Pub Date : 2022-10-05 DOI:10.1186/s42234-022-00098-8

Huan Yang, Timir Datta-Chaudhuri, Sam J George, Bilal Haider, Jason Wong, Tyler D Hepler, Ulf Andersson, Michael Brines, Kevin J Tracey, Sangeeta S Chavan

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引用次数: 0

摘要

背景：神经炎症是急性和慢性疼痛状态的重要驱动因素。因此，靶向神经炎症的分子介质可能为开发新型疼痛疗法提供机会。在神经炎性疼痛的临床前模型中，降钙素基因相关肽（CGRP）、P 物质和高迁移率组盒 1 蛋白（HMGB1）是由感觉神经元合成和释放的分子，它们会激活炎症和疼痛。高频神经电刺激（HFES）作为一种镇痛方式在临床上取得了成功，但其潜在机制尚不清楚。在此，我们推断高频电刺激可抑制感觉神经元释放神经炎症介质，从而减轻疼痛：方法：利用体外和体内试验，我们评估了 HFES 对激活的感觉神经元释放神经炎症介质的调节作用。我们在微电极阵列上培养了从表达channelrhodopsin-2（ChR2）的野生型或转基因小鼠身上获取的背根神经节（DRG）神经元，并测定了HFES对光遗传或辣椒素诱导的神经炎症介质释放的影响。此外，利用光遗传爪刺激和坐骨神经慢性收缩性损伤（CCI）神经病理性疼痛模型，在体内评估了 HFES 对局部神经炎症介质释放和痛觉减退的影响：结果：光或辣椒素诱发的神经炎症介质从培养的转基因DRG感觉神经元中释放出来，而同时进行的高频电刺激（10千赫）能显著减少神经炎症介质的释放。与这些研究结果一致的是，在光遗传刺激或CCI后，受影响爪部检测到神经炎症介质水平升高，而使用高频电刺激（20.6千赫，10分钟）每天一次，持续3天后，神经炎症介质水平升高明显减弱：这些研究揭示了高频电刺激在急性和慢性神经损伤情况下具有疼痛调节作用的一种之前尚未发现的机制。这些研究结果支持这样一种机理观点，即高频电刺激可通过抑制神经炎症介质的释放，将感觉神经元重置到较低的促炎症状态，从而减轻炎症和疼痛。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

High-frequency electrical stimulation attenuates neuronal release of inflammatory mediators and ameliorates neuropathic pain.

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High-frequency electrical stimulation attenuates neuronal release of inflammatory mediators and ameliorates neuropathic pain.

Background: Neuroinflammation is an important driver of acute and chronic pain states. Therefore, targeting molecular mediators of neuroinflammation may present an opportunity for developing novel pain therapies. In preclinical models of neuroinflammatory pain, calcitonin gene-related peptide (CGRP), substance P and high mobility group box 1 protein (HMGB1) are molecules synthesized and released by sensory neurons which activate inflammation and pain. High-frequency electrical nerve stimulation (HFES) has achieved clinical success as an analgesic modality, but the underlying mechanism is unknown. Here, we reasoned that HFES inhibits neuroinflammatory mediator release by sensory neurons to reduce pain.

Methods: Utilizing in vitro and in vivo assays, we assessed the modulating effects of HFES on neuroinflammatory mediator release by activated sensory neurons. Dorsal root ganglia (DRG) neurons harvested from wildtype or transgenic mice expressing channelrhodopsin-2 (ChR2) were cultured on micro-electrode arrays, and effect of HFES on optogenetic- or capsaicin-induced neuroinflammatory mediator release was determined. Additionally, the effects of HFES on local neuroinflammatory mediator release and hyperalgesia was assessed in vivo using optogenetic paw stimulation and the neuropathic pain model of chronic constriction injury (CCI) of the sciatic nerve.

Results: Light- or capsaicin-evoked neuroinflammatory mediator release from cultured transgenic DRG sensory neurons was significantly reduced by concurrent HFES (10 kHz). In agreement with these findings, elevated levels of neuroinflammatory mediators were detected in the affected paw following optogenetic stimulation or CCI and were significantly attenuated using HFES (20.6 kHz for 10 min) delivered once daily for 3 days.

Conclusion: These studies reveal a previously unidentified mechanism for the pain-modulating effect of HFES in the setting of acute and chronic nerve injury. The results support the mechanistic insight that HFES may reset sensory neurons into a less pro-inflammatory state via inhibiting the release of neuroinflammatory mediators resulting in reduced inflammation and pain.

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来源期刊

Bioelectronic medicine

CiteScore

6.90

自引率

0.00%

发文量

审稿时长

8 weeks