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首页> 外文期刊>Neurobiology of disease >Vagus nerve stimulation suppresses acute noxious activation of trigeminocervical neurons in animal models of primary headache
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Vagus nerve stimulation suppresses acute noxious activation of trigeminocervical neurons in animal models of primary headache

机译:迷走神经刺激抑制了在原发性头痛的动物模型中的三脑菌神经元的急性有害激活

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Abstract Vagus nerve stimulation (VNS) has been reported to be effective in the abortive treatment of both migraine and cluster headache. Using validated animal models of acute dural-intracranial (migraine-like) and trigeminal-autonomic (cluster-like) head pain we tested whether VNS suppresses ongoing and nociceptive-evoked firing of trigeminocervical neurons to explain its abortive effects in migraine and cluster headache. Unilateral VNS was applied invasively via hook electrodes placed on the vagus nerve. A single dose of ipsilateral or contralateral VNS, to trigeminal recording and dural-stimulating side, suppressed ongoing spontaneous and noxious dural-evoked trigeminocervical neuronal firing. This effect was dose-dependent, with two doses of ipsilateral VNS prolonging suppression of ongoing spontaneous firing (maximally by ~ 60%) for up to three hours, and dural-evoked (Aδ-fiber; by ~ 22%, C-fiber: by ~ 55%) responses for at least two hours. Statistically, there was no difference between ipsilateral and contralateral groups. Two doses of VNS also suppressed superior salivatory nucleus-evoked trigeminocervical neuronal responses (maximally by ~ 22%) for 2.5 h, to model nociceptive activation of the trigeminal-autonomic pathway. VNS had no effect on normal somatosensory cutaneous facial responses throughout. These studies provide a mechanistic rationale for the observed benefits of VNS in the abortive treatment of migraine and cluster headache. In addition, they further validate these preclinical models as suitable approaches to optimize therapeutic efficacy, and provide an opportunity to hypothesize and dissect the neurobiological mechanisms of VNS in the treatment of primary headaches. Highlights ? Clinical trials suggest VNS may be effective in the abortive treatment of migraine and cluster headache. ? In preclinical models VNS inhibits basal firing and nociceptive activation of trigeminocervical neurons. ? This effect is dose-dependent, but independent of laterality of stimulation side. ? These data provide a neurobiological rationale for the use of VNS in headache, and a platform to further dissect mechanisms involved.
机译:据报道,摘要迷走神经刺激(VNS)在偏头痛和群体头痛的中止治疗中有效。使用验证的动物模型的急性Dural颅内(偏头痛)和三叉动物 - 自主术(簇状)头部疼痛,我们测试了VNS是否抑制了Trigeminercace神经元的持续和伤害诱发的射击,以解释其在偏头痛和簇头痛中的造成效果。通过放置在迷走神经上的钩电极,单侧VNS被侵蚀地应用。单剂量的同侧或对侧VNS,以三血管记录和多云刺激侧,抑制了持续的自发性和有害的多云诱发的三噬菌性神经元烧制。这种效果是剂量依赖性的,用两种剂量的同侧VN延长抑制持续的自发烧制(最大〜60%),最多3小时,并且诱发(Aδ-纤维;〜22%,C-纤维: 〜55%)应对至少两个小时的反应。统计上,同侧和对侧群之间没有差异。两种剂量的VN也抑制了优异的唾液核诱导的三噬菌体神经元响应(最大〜22%)2.5小时,以模拟三叉动物自主途径的伤害活化。 VNS在始终没有对正常的躯体感应面部反应产生影响。这些研究为VNS中观察到的偏头痛和簇头痛的血管治疗中观察到的益处提供了机械理由。此外,它们进一步验证了这些临床前模型作为优化治疗效果的合适方法,并提供了假设和剖析VNS治疗原发性头痛的神经生物学机制的机会。强调 ?临床试验表明VNS可能有效地在偏头痛和簇头痛的中止治疗中有效。还在临床前模型中,VNS抑制基因截止菌神经元的基底烧制和伤害激活。还这种效果是剂量依赖性的,但与刺激侧的肤色无关。还这些数据提供了用于在头痛中使用VN的神经生物学理由,以及用于进一步解剖机制的平台。

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