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Development of CGRP-dependent pain and headache related behaviours in a rat model of concussion: Implications for mechanisms of post-traumatic headache

机译:在脑大鼠大鼠模型中依赖CGRP依赖性疼痛和头痛相关行为的发展:对后创伤后头痛机制的影响

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Background and objective Posttraumatic headache (PTH) is one of the most common, debilitating and difficult symptoms to manage after a mild traumatic brain injury, or concussion. However, the mechanisms underlying PTH remain elusive, in part due to the lack of a clinically relevant animal model. Here, we characterized for the first time, headache and pain-related behaviours in a rat model of concussion evoked by a mild closed head injury (mCHI) – the major type of military and civilian related trauma associated with PTH – and tested responses to current and novel headache therapies. Methods Concussion was induced in adult male rats using a weight-drop device. Characterization of headache and pain related behaviours included assessment of cutaneous tactile pain sensitivity, using von Frey monofilaments, and ongoing pain using the conditioned place preference or aversion (CPP/CPA) paradigms. Sensitivity to headache/migraine triggers was tested by exposing rats to low-dose glyceryl trinitrate (GTN). Treatments included acute systemic administration of sumatriptan and chronic systemic administration of a mouse anti-CGRP monoclonal antibody. Results Concussed rats developed cephalic tactile pain hypersensitivity that was resolved by two weeks post-injury and was ameliorated by treatment with sumatriptan or anti-CGRP monoclonal antibody. Sumatriptan also produced CPP seven days post mCHI, but not in sham animals. Following the resolution of the concussion-evoked cephalic hypersensitivity, administration of GTN produced a renewed and pronounced cephalic pain hypersensitivity that was inhibited by sumatriptan or anti-CGRP antibody treatment as well as a CGRP-dependent CPA. GTN had no effect in sham animals. Conclusions Concussion leads to the development of headache and pain-related behaviours, in particular sustained enhanced responses to GTN, that are mediated through a CGRP-dependent mechanism. Treatment with anti-CGRP antibodies may be a useful approach to treat PTH.
机译:背景和目的后头痛(Pth)是在轻度创伤性脑损伤或脑震荡后管理最常见,衰弱和困难的症状之一。然而,基础的机制仍然是由于缺乏临床相关的动物模型而难以捉摸。在这里,我们的特征在于,由轻度闭头损伤(MCHI)引起的大鼠震动的大鼠震动中的头痛和疼痛相关行为 - 与PTH相关的主要类型的军事和平民相关创伤 - 并对当前的反应进行了测试和新的头痛治疗。方法使用重量滴装置在成年阳性大鼠中诱发脑震荡。头痛和疼痛相关行为的表征包括使用von frey monofilamentes的皮肤触觉疼痛敏感性的评估,以及使用条件偏好或厌恶(cpp / cpa)范式的持续疼痛。通过将大鼠暴露于低剂量糖甘油(GTN)来测试对头痛/偏头痛触发器的敏感性。治疗包括血抗原和慢性全身施用小鼠抗CGRP单克隆抗体的急性全身施用。结果展示大鼠开发了损伤后两周的头孢杆触感超敏反应,并通过苏抗原或抗CGRP单克隆抗体治疗而改善。 Sumatriptan还在MCHI后七天生产CPP,但不是假动物。在解决肠道诱发的头孢菌超敏反应后,GTN的给药产生了由Sumatriptan或抗CGRP抗体治疗以及CGRP依赖性CPA抑制的更新和明显的头部疼痛超敏反应。 GTN在假动物没有影响。结论脑震荡导致头痛和疼痛相关行为的发展,特别是通过CGRP依赖机制介导的GTN的持续增强的反应。用抗CGRP抗体治疗可能是治疗PTH的有用方法。

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