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尼麦角林抑制大鼠离体海马CA1锥体神经元中的T型钙通道。

Nicergoline inhibits T-type Ca2+ channels in rat isolated hippocampal CA1 pyramidal neurones.

作者信息

Takahashi K, Akaike N

机构信息

Department of Neurophysiology, Tohoku University School of Medicine, Sendai, Japan.

出版信息

Br J Pharmacol. 1990 Aug;100(4):705-10. doi: 10.1111/j.1476-5381.1990.tb14079.x.

Abstract
  1. The effects of nicergoline on the T- and L-type Ca2+ currents in pyramidal cells freshly isolated from rat hippocampal CA1 region were investigated by use of a 'concentration-clamp' technique. The technique combines a suction-pipette technique, which allows intracellular perfusion under a single-electrode voltage-clamp, and rapid exchange of extracellular solution within 2 ms. 2. T-type Ca2+ currents were evoked by step depolarizations from a holding potential of -100 mV to potentials more positive than -70 to -60 mV, and reached a peak at about -30 mV in the current-voltage relationship. Activation and inactivation of T-type Ca2+ currents were highly potential-dependent. 3. Nicergoline and other Ca2+ antagonists dose-dependently blocked the T-type Ca2+ channel with an order of potency nicardipine greater than nicergoline greater than diltiazem. 4. The L-type Ca2+ channel was also blocked in the order nicardipine greater than nicergoline greater than diltiazem, although the T-type Ca2+ channel was more sensitive to nicergoline. 5. The inhibitory effects of nicergoline and nicardipine on the T-type Ca2+ current were voltage-, time-, and use-dependent, and the inhibition increased with a decrease in the external Ca2+ concentration. Diltiazem showed only a use-dependent block.
摘要
  1. 采用“浓度钳制”技术,研究了尼麦角林对从大鼠海马CA1区新鲜分离的锥体细胞中T型和L型Ca2+电流的影响。该技术结合了吸液管技术,可在单电极电压钳制下进行细胞内灌注,并能在2毫秒内快速更换细胞外溶液。2. T型Ca2+电流由从-100 mV的钳制电位逐步去极化至比-70至-60 mV更正的电位诱发,在电流-电压关系中,约在-30 mV时达到峰值。T型Ca2+电流的激活和失活高度依赖电位。3. 尼麦角林和其他Ca2+拮抗剂呈剂量依赖性地阻断T型Ca2+通道,其效力顺序为尼卡地平大于尼麦角林大于地尔硫䓬。4. L型Ca2+通道也按尼卡地平大于尼麦角林大于地尔硫䓬的顺序被阻断,尽管T型Ca2+通道对尼麦角林更敏感。5. 尼麦角林和尼卡地平对T型Ca2+电流的抑制作用呈电压、时间和使用依赖性,且随着细胞外Ca2+浓度的降低,抑制作用增强。地尔硫䓬仅表现出使用依赖性阻断。

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