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首页> 外文期刊>Journal of Neurophysiology >High-voltage-activated calcium current subtypes in mouse DRG neurons adapt in a subpopulation-specific manner after nerve injury
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High-voltage-activated calcium current subtypes in mouse DRG neurons adapt in a subpopulation-specific manner after nerve injury

机译:小鼠DRG神经元中的高电压激活钙电流亚型在神经损伤后以亚群特异性方式适应

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Changes in ion channel function and expression are characteristic of neuropathic pain. Voltage-gated calcium channels (VGCCs) are integral for neurotransmission and membrane excitability, but relatively little is known about changes in their expression after nerve injury. In this study, we investigate whether peripheral nerve ligation is followed by changes in the density and proportion of high-voltage-activated (HVA) VGCC current subtypes in dorsal root ganglion (DRG) neurons, the contribution of presynaptic N-type calcium channels in evoked excitatory postsynaptic currents (EPSCs) recorded from dorsal horn neurons in the spinal cord, and the changes in expression of mRNA encoding VGCC subunits in DRG neurons. Using C57BL/6 mice [8-to 11-wkold males (n = 91)] for partial sciatic nerve ligation or sham surgery, we performed whole cell patch-clamp recordings on isolated DRG neurons and dorsal horn neurons and measured the expression of all VGCC subunits with RT-PCR in DRG neurons. After nerve injury, the density of P/Q-type current was reduced overall in DRG neurons. There was an increase in the percentage of N-type and a decrease in that of P/Q-type current in medium-to large-diameter neurons. No changes were found in the contribution of presynaptic N-type calcium channels in evoked EPSCs recorded from dorsal horn neurons. The alpha 2 delta-1 subunit was upregulated by 1.7-fold and gamma-3, gamma-2, and beta-4 subunits were all downregulated 1.7-fold in injured neurons compared with sham-operated neurons. This comprehensive characterization of HVA VGCC subtypes in mouse DRG neurons after nerve injury revealed changes in N- and P/Q-type current proportions only in medium-to large-diameter neurons.
机译:离子通道功能和表达的变化是神经性疼痛的特征。电压门控钙通道(VGCC)是神经传递和膜兴奋性所不可或缺的,但对神经损伤后其表达变化的了解相对较少。在这项研究中,我们调查了背根神经节(DRG)神经元中高压激活(HVA)VGCC当前亚型的密度和比例,突触前N型钙离子通道的贡献是否与周围神经结扎有关。引起脊髓背角神经元记录的兴奋性突触后突触电流(EPSC),以及DRG神经元中编码VGCC亚基的mRNA表达的变化。使用C57BL / 6小鼠[8至11周龄雄性(n = 91)]进行部分坐骨神经结扎或假手术,我们对分离的DRG神经元和背角神经元进行了全细胞膜片钳记录,并测量了所有DRG神经元中具有RT-PCR的VGCC亚基。神经损伤后,DRG神经元的P / Q型电流密度总体降低。在中型至大直径神经元中,N型电流的百分比增加,而P / Q型电流的百分比减少。从背角神经元记录的诱发的EPSC中突触前N型钙通道的贡献未发现变化。与假手术神经元相比,受损神经元中的alpha 2 delta-1亚基上调了1.7倍,γ-3,γ-2和β-4亚基都下调了1.7倍。神经损伤后小鼠DRG神经元中HVA VGCC亚型的这种全面表征揭示了仅在中至大直径神经元中N和P / Q型电流比例发生了变化。

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