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首页> 外文期刊>Neuroscience: An International Journal under the Editorial Direction of IBRO >Nerve injury-induced changes in opioid modulation of wide dynamic range dorsal column nuclei neurones.
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Nerve injury-induced changes in opioid modulation of wide dynamic range dorsal column nuclei neurones.

机译:神经损伤引起的广泛动态范围的背柱核神经元阿片样物质调节变化。

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In the present study we investigated the effects of spinal morphine on the electrically and naturally evoked responses of gracile nuclei neurones in a rat model of neuropathy, induced by the tight ligation of lumbar L5/6 spinal nerves. Two weeks after surgery, animals were prepared for electrophysiological recordings and neuronal responses were characterised to a range of controlled natural (brush, low- and high-intensity von Frey filaments, heat 45 degrees C) and peripheral electrical stimuli. Morphine (0.1, 0.25, 1 and 5 microg) was applied spinally and its effect was compared to that in sham-operated or naive animals.Following surgery, all neuropathic rats exhibited signs of mechanical allodynia. Nerve injury induced a significant increase in the receptive field size of gracile nuclei neurones, and also produced a non-significant increase in the proportion and level of spontaneous activity in these neurones. The baseline electrical and natural evoked responses remained unaltered. Spinal morphine reduced both the Adelta-fibre- and C-fibre-evoked responses of gracile nuclei neurones, and similarly inhibited the heat-evoked responses of neuropathic, sham-operated and naive rats. Morphine, however, produced only minor reductions (<30% inhibition of pre-drug control responses) of the Abeta-fibre- and brush-evoked responses of gracile nuclei neurones. These drug effects were similar in all animal groups. In complete contrast, morphine produced a marked inhibition of the low-intensity punctate mechanical evoked responses (von Freys 2 and 9 g) after nerve injury, an effect that was totally lacking in the sham-operated or naive animal groups. This dramatic shift was selective for the low-intensity punctate mechanical stimuli and such an effect was not seen with the noxious mechanical punctate stimulus (von Frey 75 g) where there was a modest inhibition in all groups.Our results suggest that there is plasticity in the opioid modulation of dorsal column projection pathways following spinal nerve ligation and these alterations appear to interact with sensory pathways conveying low-threshold punctate stimuli.
机译:在本研究中,我们研究了脊髓吗啡对腰椎L5 / 6脊神经紧密结扎诱导的大鼠神经病模型中柔韧核神经元电和自然诱发反应的影响。手术后两周,准备动物进行电生理记录,并根据一系列受控的自然(刷子,低强度和高强度von Frey细丝,加热45摄氏度)和周围电刺激对神经元反应进行表征。吗啡(0.1、0.25、1和5微克)经脊髓应用,其效果与假手术或幼稚动物相比。在手术后,所有神经性大鼠均表现出机械性异常性疼痛的迹象。神经损伤引起了柔韧核神经元的感受野大小的显着增加,并且在这些神经元中自发活动的比例和水平上也没有显着增加。基线电和自然诱发反应保持不变。脊髓吗啡降低了轻度核神经元的Adelta纤维和C纤维诱发的反应,并同样抑制了神经性,假手术和幼稚大鼠的热诱发反应。然而,吗啡仅使轻度神经核神经元的Abeta纤维和刷子诱发的反应产生较小的减少(<30%的药物前控制反应抑制)。在所有动物组中,这些药物作用均相似。完全相反,在神经损伤后,吗啡对低强度的点状机械诱发反应(von Freys 2和9 g)产生了明显的抑制作用,在假手术或幼稚的动物组中完全没有这种作用。这种剧烈的变化对低强度的点状机械刺激具有选择性,而在有害的机械点状刺激(von Frey 75 g)中,所有组均存在适度的抑制作用,而这种效果并未见到。脊髓神经结扎后阿片样物质对背柱投射途径的调节,这些改变似乎与传达低阈点状刺激的感觉途径相互作用。

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