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陈荣贵

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颈背根节神经元异位自发放电增强诱致大鼠慢性颈椎根性痛的作用机制研究被引量:1
2016年
目的:建立慢性压迫颈背根神经节诱致的颈椎根性痛(cervical radiculopathic pain,CRP)模型,观察颈背根节神经元产生异位自发放电诱致颈椎根性痛的作用。方法:采用体重为100~150 g的成年SD大鼠,在椎间孔内植入L型不锈钢钢柱形成慢性压迫C7/C8背根节,建立颈椎根性痛模型。用Von Frey细丝刺激大鼠前足足底来检测机械痛敏。用热辐射刺激仪刺激大鼠前足足底来检测热痛敏,其热缩足反射潜伏期由自动计时器读出。用丙酮刺激大鼠前足足底来观察冷刺激反应级别;同时检测大鼠前足肌肉的瞬间肌力;进行在体C7/C8 DRG背根纤维胞外电生理记录。结果:(1)CRP大鼠损伤侧前足表现出对机械刺激、热刺激以及冷刺激明显的痛觉过敏现象。(2)在C7/C8 DRG慢性压迫损伤后有62.7%的神经元发生异位自发放电,而对照组只有22.5%的神经元发生自发放电。与对照组相比,CRP组发生异位自发放电的比例明显增加。受损神经元的自发放电呈现三种不同的放电模式,即阵发性放电,周期性放电以及非周期性放电。结论:我们通过对C7/C8 DRG神经元施加稳固的慢性机械压迫建立了一个新的CRP模型,CRP大鼠表现出明显的痛行为学过敏反应。这种痛觉过敏可能由受损DRG神经元异位自发放电增强介导。
张昱琦陈荣贵孔微微曹智胡三觉董辉罗层
关键词:背根节触诱发痛自发放电
Bilateral mechanical and thermal hyperalgesia and tactile allodynia after chronic compression of dorsal root ganglion in mice
2011年
Objective Low back pain is one of the most inextricable problems encountered in clinics. Animal models that imitate symptoms in humans are valuable tools for investigating low back pain mechanisms and the possible therapeutic applications. With the development of genetic technology in pain field, the possibility of mutating specific genes in mice has provided a potent tool for investigating the specific mechanisms of pain. The aim of the present study was to develop a mouse model of chronic compression of dorsal root ganglion (CCD), in which gene mutation can be applied to facilitate the studies of chronic pain. Methods Chronic compression of L4 and L5 dorsal root ganglia was conducted in mice by inserting fine stainless steel rods into the intervertebral foramina, one at L4 and the other at L5. Mechanical allodynia and thermal hyperalgesia were examined with von Frey filaments and radiating heat stimulator, respectively. Results The CCD mice displayed dramatic mechanical and thermal hyperalgesia as well as tactile allodynia in the hindpaw ipsilateral to CCD. In addition, this mechanical and thermal hyperalgesia as well as tactile allodynia was also found to spread to the contralateral hindpaw. Conclusion This model, combined with the possible genetic modification, will strengthen our knowledge of the underlying mechanisms of low back pain. It also favors the development of new treatment strategies for pain and hyperalgesia after spinal injury and other disorders which affect the dorsal root ganglion in humans.
陈荣贵孔微微葛大龙罗层胡三觉
关键词:MICEHYPERALGESIAALLODYNIA
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