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Alteration by Xylocaine (Lidocaine) and Its Derivatives of the Time Course of the End Plate Potential

机译:Xylocaine(Lidocaine)及其衍生物的终极板电位时程变化

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摘要

Xylocaine and its derivatives act specifically at the neuromuscular junction within the concentration range 0.05 to 2.0 mM. The charged form is the active form of the drugs. There is no correlation between "local anesthetic" activity and effect at the junction. Like d-tubocurarine, these drugs have little or no effect on quantum content, acetylcholinesterase activity, or the passive impedance of the muscle fiber. Yet they produce end plate potentials characterized by a brief, early component and a late, greatly prolonged component, as does procaine. Analysis of these changes in time course suggests that the drugs have little or no effect before receptors are activated by acetylcholine, but cause a decreased and often greatly prolonged response. Clear structure-activity relations indicate that the receptor to which the drugs bind to produce the prolonged response can be the receptor for acetylcholine. Comparison of the effects of the drugs on the end plate potential and on the response to iontophoretically applied acetylcholine also shows that the effects of Xylocaine depend on the time course of receptor activation and are quite different from the effects of d-tubocurarine.
机译:Xylocaine及其衍生物在0.05至2.0 mM的浓度范围内特异性作用于神经肌肉接头。收费形式是药物的活性形式。 “局部麻醉”活性与交界处的作用之间没有相关性。像d-微管尿素一样,这些药物对量子含量,乙酰胆碱酯酶活性或肌纤维的被动阻抗几乎没有影响。然而,它们产生的终板电位与普鲁卡因一样,具有短暂的早期成分和晚期,大大延长的成分。对这些随时间变化的分析表明,在受体被乙酰胆碱激活之前,该药物几乎没有或没有作用,但会导致反应减少并通常大大延长反应时间。明确的结构活性关系表明与药物结合以产生延长反应的受体可以是乙酰胆碱的受体。比较药物对终板电位的影响以及对离子电渗疗法施加​​的乙酰胆碱的反应的影响,还表明,赛洛卡因的作用取决于受体激活的时间过程,与d-微管尿素的作用完全不同。

著录项

  • 作者

    Steinbach, A. B.;

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  • 年度 1968
  • 总页数
  • 原文格式 PDF
  • 正文语种 {"code":"en","name":"English","id":9}
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