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速激肽对七鳃鳗脊髓中感觉神经元、中间神经元及突触传递的调节作用

Tachykinin-mediated modulation of sensory neurons, interneurons, and synaptic transmission in the lamprey spinal cord.

作者信息

Parker D, Grillner S

机构信息

Nobel Institute for Neurophysiology, Department of Neuroscience, Karolinska Institute, Stockholm, Sweden.

出版信息

J Neurophysiol. 1996 Dec;76(6):4031-9. doi: 10.1152/jn.1996.76.6.4031.

Abstract
  1. Tachykinin-like immunoreactivity is found in the dorsal roots, dorsal horn, and dorsal column of the lamprey. The effect of tachykinins on sensory processing was examined by recording intracellularly from primary sensory dorsal cells and second-order spinobulbar giant interneurons. Modulation of synaptic transmission was examined by making paired recordings from dorsal cells and giant interneurons, or by eliciting compound depolarizations in the giant interneurons by stimulating the dorsal root or dorsal column. 2. Bath application of tachykinins depolarized the dorsal cells. This effect was mimicked by stimulation of the dorsal root, suggesting that dorsal root afferents may be a source of endogenous tachykinin input to the spinal cord. The depolarization was reduced by removal of sodium or calcium from the Ringer, or when potassium conductances were blocked, and was not associated with a measurable change in input resistance. Dorsal root stimulation also caused a depolarization in the dorsal cells, and this effect and that of bath-applied substance P, was blocked by the tachykinin antagonist spantide. 3. The tachykinin substance P could reduce inward and outward rectification in the dorsal cells, the effect on outward rectification only being seen when potassium conductances were blocked by tetraethylammonium (TEA). 4. Substance P increased the excitability of the dorsal cells and giant interneurons, shown by the increased spiking in response to depolarizing current pulses. The increased excitability was blocked by the tachykinin antagonist spantide. 5. Substance P modulated the dorsal cell action potential, by increasing the spike duration and reducing the amplitude of the afterhyperpolarization. The spike amplitude was not consistently affected. 6. Stimulation of the dorsal column resulted in either depolarizing or hyperpolarizing potentials in the giant interneurons. The amplitude of the depolarization was increased by substance P, whereas the amplitude of the hyperpolarization was reduced. These effects occurred independently of a measurable change in postsynaptic input resistance, suggesting that the modulation occurred presynaptically. Paired recordings from dorsal cells and giant interneurons failed to reveal an effect of substance P on dorsal cell-evoked excitatory postsynaptic potentials (EPSPs), suggesting that the potentiation of the dorsal column-evoked depolarization was due to an effect on other axons in the dorsal column. Dorsal root-evoked potentials could also be increased in the presence of substance P, although this effect was less consistent than the effect on dorsal column stimulation. 7. These results suggest that tachykinins modulate sensory input to the lamprey spinal cord by increasing the excitability of primary afferents and second-order giant interneurons, and also by modulating synaptic transmission. Tachykinins may result in potentiation of local spinal reflexes and also modulation of descending reticulospinal inputs to the spinal locomotor network as a result of potentiation of spinobulbar inputs.
摘要
  1. 在七鳃鳗的背根、背角和背柱中发现了速激肽样免疫反应性。通过对初级感觉背侧细胞和二级脊髓延髓巨中间神经元进行细胞内记录,研究了速激肽对感觉处理的影响。通过对背侧细胞和巨中间神经元进行配对记录,或通过刺激背根或背柱在巨中间神经元中引发复合去极化,研究了突触传递的调制。2. 浴用速激肽使背侧细胞去极化。刺激背根可模拟这种效应,表明背根传入神经可能是脊髓内源性速激肽输入的来源。去除林格氏液中的钠或钙,或阻断钾电导时,去极化作用减弱,且与输入电阻的可测量变化无关。背根刺激也会使背侧细胞去极化,这种效应以及浴用P物质的效应被速激肽拮抗剂spantide阻断。3. 速激肽P物质可降低背侧细胞的内向和外向整流,仅在四乙铵(TEA)阻断钾电导时才可见对外向整流的影响。4. P物质增加了背侧细胞和巨中间神经元的兴奋性,表现为对去极化电流脉冲的发放增加。速激肽拮抗剂spantide可阻断这种增加的兴奋性。5. P物质通过增加动作电位持续时间和减小超极化后电位的幅度来调制背侧细胞动作电位。动作电位幅度并非始终受到影响。6. 刺激背柱在巨中间神经元中产生去极化或超极化电位。P物质增加了去极化的幅度,而减小了超极化的幅度。这些效应独立于突触后输入电阻的可测量变化而发生,表明调制发生在突触前。背侧细胞和巨中间神经元的配对记录未能揭示P物质对背侧细胞诱发的兴奋性突触后电位(EPSP)的影响,表明背柱诱发的去极化增强是由于对背柱中其他轴突的作用。在存在P物质的情况下,背根诱发的电位也可能增加,尽管这种效应不如对背柱刺激的效应一致。7. 这些结果表明,速激肽通过增加初级传入神经和二级巨中间神经元的兴奋性以及调制突触传递来调节七鳃鳗脊髓的感觉输入。速激肽可能导致局部脊髓反射的增强,并且由于脊髓延髓输入的增强,也可能调制下行网状脊髓对脊髓运动网络的输入。

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