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首页> 美国卫生研究院文献>The Journal of Physiology >Peripheral nerve injury alters excitatory synaptic transmission in lamina II of the rat dorsal horn
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Peripheral nerve injury alters excitatory synaptic transmission in lamina II of the rat dorsal horn

机译:周围神经损伤改变了大鼠背角椎板II的兴奋性突触传递

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Using the blind whole cell patch-clamp recording technique, we investigated peripheral nerve injury-induced changes in excitatory synaptic transmission to neurones in lamina II of the dorsal horn. Partial (i.e. chronic constriction injury (CCI) and spared nerve injury (SNI)) and complete (i.e. sciatic nerve transection (SNT)) peripheral nerve injury altered the mean threshold intensity for eliciting A fibre-mediated EPSCs in lamina II neurones. Following SNT and CCI, EPSC threshold was significantly decreased, but following SNI, EPSC threshold was increased (naive: 32 ± 2 μA, SNT: 22 ± 2 μA, CCI: 23 ± 2 μA, SNI: 49 ± 4 μA; P < 0.01, Student's unpaired t test). Despite this disparity between models, dorsal root compound action potential recordings revealed no significant difference in the conduction velocity or activation threshold of Aβ and Aδ fibres in naive, SNT, CCI and SNI rats. In addition to the changes in EPSC threshold, we also observed a shift in the distribution of EPSCs. In spinal cord slices from naive rats, polysynaptic Aβ fibre-evoked EPSCs were observed in 24 % of lamina II neurones, monosynaptic Aδ fibre EPSCs were observed in 34 % and polysynaptic Aδ fibre EPSCs were observed in 7 %. Following SNT and CCI, the percentage of neurones with polysynaptic Aβ fibre EPSCs increased to ≥ 65 % of the sampled population, while the percentage of neurones with monosynaptic Aδ fibre EPSCs decreased to < 10 %. The percentage of neurones with polysynaptic Aδ fibre EPSCs was unchanged. In contrast, following SNI, Aβ fibre EPSCs decreased in incidence while the percentage of neurones with polysynaptic Aδ fibre EPSCs increased to 44 %. Similar to the other injury models, however, monosynaptic Aδ fibre EPSCs decreased in frequency following SNI. Thus, excitatory synaptic transmission is subject to divergent plasticity in different peripheral nerve injury models, reflecting the complexity of responses to different forms of deafferentation.
机译:使用盲全细胞膜片钳记录技术,我们调查了周围神经损伤引起的兴奋性突触传递到背角板层II神经元的突触变化。部分(即慢性收缩损伤(CCI)和神经损伤(SNI))和完全(即坐骨神经横切(SNT))周围神经损伤改变了在层II神经元中引起A纤维介导的EPSC的平均阈值强度。在SNT和CCI之后,EPSC阈值显着降低,但在SNI之后,EPSC阈值增加(天真:32±2μA,SNT:22±2μA,CCI:23±2μA,SNI:49±4μA; P < 0.01,学生的未配对t检验)。尽管模型之间存在差异,但背根复合动作电位记录显示,在幼稚,SNT,CCI和SNI大鼠中,Aβ和Aδ纤维的传导速度或激活阈值无显着差异。除了EPSC阈值的变化外,我们还观察到EPSC分布的变化。在幼稚大鼠的脊髓切片中,在24%的lamina II神经元中观察到多突触Aβ纤维诱发的EPSC,在34%中观察到单突触Aδ纤维EPSC,在7%中观察到多突触Aδ纤维EPSC。进行SNT和CCI后,具有多突触Aβ纤维EPSC的神经元的百分比增加到抽样人群的≥65%,而具有单突触Aδ纤维EPSC的神经元的百分比降低到<10%。具有多突触Aδ纤维EPSC的神经元的百分比不变。相反,在SNI后,Aβ纤维EPSC的发生率降低,而具有多突触Aδ纤维EPSC的神经元的百分比增加到44%。但是,与其他损伤模型相似,SNI后单突触Aδ纤维EPSC的频率降低。因此,在不同的周围神经损伤模型中,兴奋性突触传递受不同的可塑性影响,反映了对不同形式的脱除咖啡因的反应的复杂性。

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