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Assessing the role of IKCa channels in generating the sAHP of CA1 hippocampal pyramidal cells

机译:评估IKCa通道在产生CA1海马锥体细胞sAHP中的作用

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摘要

Our previous work reported that KCa3.1 (IKCa) channels are expressed in CA1 hippocampal pyramidal cells and contribute to the slow afterhyperpolarization that regulates spike accommodation in these cells. The current report presents data from single cell RT-PCR that further reveals mRNA in CA1 cells that corresponds to the sequence of an IKCa channel from transmembrane segments 5 through 6 including the pore region, revealing the established binding sites for 4 different IKCa channel blockers. A comparison of methods to internally apply the IKCa channel blocker TRAM-34 shows that including the drug in an electrode from the onset of an experiment is unviable given the speed of drug action upon gaining access for whole-cell recordings. Together the data firmly establish IKCa channel expression in CA1 neurons and clarify methodological requirements to obtain a block of IKCa channel activity through internal application of TRAM-34.
机译:我们以前的工作报道,KCa3.1(IKCa)通道在CA1海马锥体细胞中表达,并且有助于调节这些细胞中的突波适应性的缓慢超极化。本报告提供了来自单细胞RT-PCR的数据,该数据进一步揭示了CA1细胞中的mRNA,该mRNA与来自跨膜片段5至6的IKCa通道序列(包括孔区域)相对应,揭示了针对4种不同的IKCa通道阻滞剂建立的结合位点。对内部应用IKCa通道阻滞剂TRAM-34的方法的比较表明,考虑到获得全细胞记录时药物作用的速度,从实验开始就将药物包含在电极中是不可行的。这些数据一起牢固地建立了CA1神经元中IKCa通道的表达,并阐明了通过内部应用TRAM-34获得IKCa通道活性的方法学要求。

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