首页> 美国卫生研究院文献>The Journal of Neuroscience >Functional and Molecular Differences between Voltage-Gated K+ Channels of Fast-Spiking Interneurons and Pyramidal Neurons of Rat Hippocampus
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Functional and Molecular Differences between Voltage-Gated K+ Channels of Fast-Spiking Interneurons and Pyramidal Neurons of Rat Hippocampus

机译:大鼠海马快速加标中枢神经元的电压门控K +通道和锥体神经元之间的功能和分子差异

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摘要

We have examined gating and pharmacological characteristics of somatic K+ channels in fast-spiking interneurons and regularly spiking principal neurons of hippocampal slices. In nucleated patches isolated from basket cells of the dentate gyrus, a fast delayed rectifier K+ current component that was highly sensitive to tetraethylammonium (TEA) and 4-aminopyridine (4-AP) (half-maximal inhibitory concentrations <0.1 mm) predominated, contributing an average of 58% to the total K+ current in these cells. By contrast, in pyramidal neurons of the CA1 region a rapidly inactivating A-type K+ current component that was TEA-resistant prevailed, contributing 61% to the total K+current. Both types of neurons also showed small amounts of the K+ current component mainly found in the other type of neuron and, in addition, a slow delayed rectifier K+ current component with intermediate properties (slow inactivation, intermediate sensitivity to TEA). Single-cell RT-PCR analysis of mRNA revealed that Kv3 (Kv3.1, Kv3.2) subunit transcripts were expressed in almost all (89%) of the interneurons but only in 17% of the pyramidal neurons. In contrast, Kv4 (Kv4.2, Kv4.3) subunit mRNAs were present in 87% of pyramidal neurons but only in 55% of interneurons. Selective block of fast delayed rectifier K+ channels, presumably assembled from Kv3 subunits, by 4-AP reduced substantially the action potential frequency in interneurons. These results indicate that the differential expression of Kv3 and Kv4 subunits shapes the action potential phenotypes of principal neurons and interneurons in the cortex.
机译:我们研究了快速加标的中间神经元和定期加标海马切片的主要神经元的体细胞K + 通道的门控和药理特性。在从齿状回的篮状细胞中分离出的有核斑块中,快速延迟的整流器K + 电流成分对四乙铵(TEA)和4-氨基吡啶(4-AP)高度敏感(半最大抑制浓度<0.1 mm)占主导地位,平均贡献了这些电池中总K + 电流的58%。相比之下,在CA1区的锥体神经元中,快速失活的TE型抗性A型K + 电流成分占主导地位,占总K + 电流的61% 。两种类型的神经元也都显示出少量的K + 电流分量,主要存在于其他类型的神经元中,此外,还有一个缓慢延迟的整流器K + 电流分量,具有中等性质(缓慢失活,对TEA的中等敏感性)。 mRNA的单细胞RT-PCR分析显示,Kv3(Kv3.1,Kv3.2)亚基转录本在几乎所有(89%)的中间神经元中表达,但仅在17%的锥体神经元中表达。相反,Kv4(Kv4.2,Kv4.3)亚基mRNA存在于87%的锥体神经元中,但仅存在于55%的中间神经元中。快速延迟整流器K + 通道的选择性阻滞,大概是由Kv3亚基通过4-AP组装而成,大大降低了中间神经元的动作电位频率。这些结果表明Kv3和Kv4亚基的差异表达塑造了皮层中主要神经元和中间神经元的动作电位表型。

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