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首页> 外文期刊>The Royal Society Proceedings B: Biological Sciences >Different calcium channels are coupled to potassium channels with distinct physiological roles in vagal neurons.
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Different calcium channels are coupled to potassium channels with distinct physiological roles in vagal neurons.

机译:在迷走神经元中,不同的钙通道与具有独特生理作用的钾通道偶联。

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摘要

Whole-cell and sharp microelectrode recordings were obtained from neurons of rat dorsal motor nucleus of the vagus (DMV) in transverse slices of the rat medulla maintained in vitro. Calcium currents were studied with sodium currents blocked with tetrodotoxin, potassium currents blocked by perfusing the cell with caesium as the main cation and using barium as the charge carrier. From a holding potential of -60 mV, inward currents activated at potentials positive of -50 mV and peaked around 0 mV. Voltage clamping the neuron at more hyperpolarised potentials did not reveal any low-threshold inward current. The inward current was effectively blocked by cadmium (100 microM) and nicked (1 mM), suggesting that it is carried by voltage-dependent calcium channels. The inward current could be separated into three pharmacologically distinct components: 40% of the whole cell current was omega-conotoxin sensitive; 20% of the current was nifedipine sensitive; and the rest was blocked by high concentrations of cadmium and nickel. This remaining current cannot be due to P-type calcium channels as omega-agatoxin had no effect on the inward current. Nifedipine had no significant effect on the action potential. Application of omega-conotoxin reduced the calcium component of the action potential and significantly reduced the potassium current underlying the afterhyperpolarization. Application of charybdotoxin slowed action potential repolarization. When N-type calcium channels were blocked with omega-conotoxin, charybdotoxin was still effective in slowing repolarization. In contrast, charybdotoxin was ineffective ineffective when calcium influx was blocked with the non-specific calcium channel blocker cadmium.(ABSTRACT TRUNCATED AT 250 WORDS)
机译:从在体外维持的大鼠延髓横切片的迷走神经大鼠背运动核神经元(DMV)的神经元中获得全细胞和清晰的微电极记录。研究了钙电流,河豚毒素阻断的钠电流,通过以铯为主要阳离子灌注细胞并以钡为电荷载体阻断钾电流的研究。从-60 mV的保持电势开始,流入电流以-50 mV的正电势激活,并在0 mV附近达到峰值。将神经元钳位在更多的超极化电位上的电压并未显示出任何低阈值的内向电流。流入电流有效地被镉(100 microM)阻挡并形成切口(1 mM),这表明它是由电压依赖性钙通道携带的。内向电流可分为三个药理学上不同的成分:40%的全细胞电流对ω-芋螺毒素敏感;目前有20%对硝苯地平敏感;其余的则被高浓度的镉和镍所阻挡。该剩余电流不能归因于P型钙通道,因为ω-毒素对内向电流没有影响。硝苯地平对动作电位无明显影响。 ω-芋螺毒素的应用降低了动作电位的钙成分,并大大降低了超极化后的钾电流。炭疽毒素的应用减缓了动作电位的复极。当N型钙通道被ω-芋螺毒素所阻断时,炭疽毒素仍然可以有效地减缓复极化。相反,当用非特异性钙通道阻滞剂镉阻止钙流入时,炭疽毒素无效。(摘要截断为250个字)

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