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青蛙骨骼肌纤维中的收缩失活。低钙、丁卡因、丹曲林、D - 600和硝苯地平的作用。

Contractile inactivation in frog skeletal muscle fibers. The effects of low calcium, tetracaine, dantrolene, D-600, and nifedipine.

作者信息

Caputo C, Bolaños P

出版信息

J Gen Physiol. 1987 Mar;89(3):421-42. doi: 10.1085/jgp.89.3.421.

Abstract

Short muscle fibers (approximately 1.5 mm) of Rana pipiens were voltage-clamped with a two-microelectrode technique at a holding potential of -100 mV. Using conditioning depolarizing ramps, with slopes greater than 0.2 mV/s, partially inactivated responses are obtained at threshold values between -55 and -35 mV. With slopes equal to or slower than 0.1 mV/s, one inactivates contraction without ever activating it. When the membrane potential is brought slowly to values more positive than about -40 mV, test pulses, applied on top of the ramps, bringing the membrane potential to values up to +100 mV, are ineffective in eliciting contractile responses, which indicates complete inactivation. After inactivation, contractile threshold is shifted by perhaps 10 mV, to about -40 mV. The sensitivity of fibers to depolarizing ramps is increased by D-600 (50 microM), dantrolene (50 microM), tetracaine (100 microM), and low calcium (10(-8) M). In the presence of these agents, complete inactivation was obtained using ramp slopes of 1, 0.8, 0.4, and 0.2 mV/s, respectively. Nifedipine was less effective. With D-600, once inactivation had been induced, no repriming occurred after repolarization to -100 mV, and partial recovery occurred after washing out the drug. With low calcium, tetracaine, and nifedipine, the tension-voltage relationship was not affected, whereas the steady state inactivation curve (obtained in repriming experiments) was shifted by 10-25 mV toward more negative potentials. With D-600, the activation curve was not modified, whereas the inactivation curve could not be obtained, because of repriming failure. With dantrolene, the inactivation curve was not affected, whereas the activation curve was shifted toward less negative potentials and peak tension diminished, depending on the pulse duration. The results indicate that it is possible to induce complete inactivation without activation, and to differentiate activation and inactivation parameters pharmacologically, which suggests that the two are separate processes.

摘要

用双微电极技术在-100 mV的钳制电位下对牛蛙的短肌纤维(约1.5毫米)进行电压钳制。使用斜率大于0.2 mV/s的条件性去极化斜坡,在-55至-35 mV的阈值处可获得部分失活反应。当斜率等于或慢于0.1 mV/s时,可使收缩失活而不引发收缩。当膜电位缓慢升至比约-40 mV更正的值时,施加在斜坡之上、使膜电位升至+100 mV的测试脉冲无法引发收缩反应,这表明完全失活。失活后,收缩阈值可能会偏移约10 mV,至约-40 mV。D-600(50微摩尔)、丹曲林(50微摩尔)、丁卡因(100微摩尔)和低钙(10⁻⁸ M)可增加纤维对去极化斜坡的敏感性。在这些药剂存在的情况下,分别使用1、0.8、0.4和0.2 mV/s的斜坡斜率可实现完全失活。硝苯地平的效果较差。使用D-600时,一旦诱导失活,复极化至-100 mV后不会发生再激发,药物洗脱后会出现部分恢复。使用低钙、丁卡因和硝苯地平时,张力-电压关系不受影响,而稳态失活曲线(在再激发实验中获得)会向更负的电位偏移10 - 25 mV。使用D-600时,激活曲线未改变,而由于再激发失败无法获得失活曲线。使用丹曲林时,失活曲线不受影响,而激活曲线会向较不那么负的电位偏移,且峰值张力会降低,这取决于脉冲持续时间。结果表明,可以在不激活的情况下诱导完全失活,并在药理学上区分激活和失活参数,这表明两者是独立的过程。

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