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Block of single L-type Ca2+ channels in skeletal muscle fibers by aminoglycoside antibiotics

机译:氨基糖苷类抗生素阻断骨骼肌纤维中单个L型Ca2 +通道

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摘要

The activity of single L-type Ca2+ channels was recorded from cell- attached patches on acutely isolated skeletal muscle fibers from the mouse. The experiments were concerned with the mechanism by which aminoglycoside antibiotics inhibit ion flow through the channel. Aminoglycosides produced discrete fluctuations in the single-channel current when added to the external solution. The blocking kinetics could be described as a simple bimolecular reaction between an aminoglycoside molecule and the open channel. The blocking rate was found to be increased when either the membrane potential was made more negative or the concentration of external permeant ion was reduced. Both of these effects are consistent with a blocking site that is located within the channel pore. Other features of block, however, were incompatible with a simple pore blocking mechanism. Hyperpolarization enhanced the rate of unblocking, even though an aminoglycoside molecule must dissociate from its binding site in the channel toward the external solution against the membrane field. Raising the external permeant ion concentration also enhanced the rate of unblocking. This latter finding suggests that aminglycoside affinity is modified by repulsive interactions that arise when the pore is simultaneously occupied by a permeant ion and an aminoglycoside molecule.
机译:从小鼠急性分离的骨骼肌纤维上的细胞贴片中记录了单个L型Ca2 +通道的活性。实验与氨基糖苷类抗生素抑制离子流经通道的机制有关。当添加到外部溶液中时,氨基糖苷会在单通道电流中产生离散的波动。阻断动力学可以描述为氨基糖苷分子和开放通道之间的简单双分子反应。当使膜电位更负或降低外部渗透离子的浓度时,发现阻断速率增加。这两种作用均与位于通道孔内的阻断位点一致。但是,阻塞的其他特征与简单的孔阻塞机制不兼容。超极化提高了解封闭的速率,即使氨基糖苷分子必须从通道中的结合位点向膜溶液的外部溶液解离。提高外部渗透离子浓度也提高了解封率。后一个发现表明,当孔同时被一个渗透离子和一个氨基糖苷分子占据时,排斥相互作用改变了阿糖苷的亲和力。

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  • 年度 1996
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  • 正文语种 {"code":"en","name":"English","id":9}
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