首页> 外文期刊>The Journal of general physiology >The delayed rectifier potassium conductance in the sarcolemma and the transverse tubular system membranes of mammalian skeletal muscle fibers
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The delayed rectifier potassium conductance in the sarcolemma and the transverse tubular system membranes of mammalian skeletal muscle fibers

机译:哺乳动物骨骼肌纤维的肌膜和横管系统膜中的延迟整流钾电导

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A two-microelectrode voltage clamp and optical measurements of membrane potential changes at the transverse tubular system (TTS) were used to characterize delayed rectifier K currents (IKV) in murine muscle fibers stained with the potentiometric dye di-8-ANEPPS. In intact fibers, IKV displays the canonical hallmarks of KV channels: voltage-dependent delayed activation and decay in time. The voltage dependence of the peak conductance (gKV) was only accounted for by double Boltzmann fits, suggesting at least two channel contributions to IKV. Osmotically treated fibers showed significant disconnection of the TTS and displayed smaller IKV, but with similar voltage dependence and time decays to intact fibers. This suggests that inactivation may be responsible for most of the decay in IKV records. A two-channel model that faithfully simulates IKV records in osmotically treated fibers comprises a low threshold and steeply voltage-dependent channel (channel A), which contributes ~31% of gKV, and a more abundant high threshold channel (channel B), with shallower voltage dependence. Significant expression of the IKV1.4 and IKV3.4 channels was demonstrated by immunoblotting. Rectangular depolarizing pulses elicited step-like di-8-ANEPPS transients in intact fibers rendered electrically passive. In contrast, activation of IKV resulted in time- and voltage-dependent attenuations in optical transients that coincided in time with the peaks of IKV records. Normalized peak attenuations showed the same voltage dependence as peak IKV plots. A radial cable model including channels A and B and K diffusion in the TTS was used to simulate IKV and average TTS voltage changes. Model predictions and experimental data were compared to determine what fraction of gKV in the TTS accounted simultaneously for the electrical and optical data. Best predictions suggest that KV channels are approximately equally distributed in the sarcolemma and TTS membranes; under these conditions, 70% of IKV arises from the TTS.
机译:使用两微电极电压钳和横向管状系统(TTS)的膜电势变化的光学测量来表征用电位染料di-8-ANEPPS染色的鼠肌纤维中的延迟整流K电流(IKV)。在完整的光纤中,IKV会显示KV通道的典型标志:依赖电压的延迟激活和时间衰减。峰值电导(gKV)的电压依赖性仅由双Boltzmann拟合来解释,这表明至少有两个通道对IKV有贡献。经渗透处理的纤维表现出TTS的显着断开,并显示出较小的IKV,但对完整纤维的电压依赖性和时间衰减相似。这表明灭活可能是IKV记录中大部分衰减的原因。一个忠实地模拟经渗透处理的光纤中的IKV记录的两通道模型包括一个低阈值和陡峭的电压相关通道(通道A),贡献了约31%的gKV,一个更丰富的高阈值通道(通道B),较浅的电压依赖性。通过免疫印迹证实了IKV1.4和IKV3.4通道的显着表达。矩形去极化脉冲会在完整的光纤中产生阶跃状的di-8-ANEPPS瞬变,从而使电被动。相反,IKV的激活导致光学瞬态的时间和电压相关衰减,这些衰减在时间上与IKV记录的峰值一致。归一化的峰值衰减显示出与峰值IKV图相同的电压依赖性。使用包含TTS中通道A和B以及K扩散的径向电缆模型来模拟IKV和平均TTS电压变化。比较了模型预测和实验数据,以确定TTS中gKV的哪些部分同时反映了电学和光学数据。最好的预测表明,KV通道在肌膜和TTS膜中分布大致相等。在这些条件下,超过70%的IKV来自TTS。

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