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Effect of trimebutine on voltage-activated calcium current in rabbit ileal smooth muscle cells.

机译:曲美布汀对家兔回肠平滑肌细胞电压激活钙电流的影响。

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摘要

1. The effect of trimebutine on the voltage-dependent inward Ca2+ current was investigated by the whole-cell voltage-clamp technique in single smooth muscle cells from rabbit ileum. 2. Trimebutine (3-100 microM) reduced the Ca2+ current in a concentration-dependent manner. The inhibitory effect on the Ca2+ current was also dependent on the holding potential. The Ca2+ current after a low holding potential was inhibited to a greater extent than that after a high membrane potential: the IC50 values were 7 microM and 36 microM at holding potentials of -40 mV and -60 mV, respectively. The Ca2+ current elicited from a holding potential of -80 mV could not be reduced by as much as 50% of the control by trimebutine at concentrations as high as 100 microM. 3. Trimebutine (30 microM) shifted the voltage-dependent inactivation curve for the Ca2+ current by 18 mV in the negative direction. The affinity of the drug for Ca2+ channels was calculated to be 36 times higher in the inactivated state than in the closed-available state. 4. Blockade of the Ca2+ current by trimebutine, unlike verapamil, was not use-dependent. 5. The results suggest that trimebutine inhibits the voltage-dependent inward Ca2+ current through a preferential binding to Ca2+ channels in the inactivated state in the smooth muscle cell from rabbit ileum. The inhibitory effect of trimebutine on gastrointestinal motility is discussed in the light of the present findings.
机译:1.通过全细胞电压钳技术研究了兔回肠单个平滑肌细胞中曲美布汀对电压依赖性内向Ca2 +电流的影响。 2. Trimebutine(3-100 microM)以浓度依赖性方式降低Ca2 +电流。对Ca2 +电流的抑制作用还取决于保持电位。低保持电位后的Ca2 +电流受到抑制的程度比高膜电位后更大:在-40 mV和-60 mV的保持电位下,IC50值分别为7 microM和36 microM。由-80 mV的保持电位引起的Ca2 +电流在100μM的浓度下不能被曲美布汀减少多达对照的50%。 3. Trimebutine(30 microM)使Ca2 +电流的电压依赖性灭活曲线在负方向上移动了18 mV。计算出的药物对Ca2 +通道的亲和力在灭活状态下比在封闭状态下高36倍。 4.与维拉帕米不同,曲美布汀对Ca2 +电流的阻断作用与使用无关。 5.结果表明曲美布汀通过优先结合兔回肠平滑肌细胞中处于灭活状态的Ca2 +通道,从而抑制了电压依赖性内向Ca2 +电流。根据目前的发现,讨论了曲美布汀对胃肠蠕动的抑制作用。

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