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预充罗库溴铵:与罗库溴铵和米库氯铵的比较。

Priming rapacuronium: a comparison with rocuronium and mivacurium.

作者信息

Steinberg David

机构信息

Hospital de Clínicas Caracas, Servicio de Anestesiología, San Bernandino Caracas, Venezuela.

出版信息

Acta Cient Venez. 2003;54(2):115-20.

Abstract

The aim of this study is to present the pharmacodynamics of the priming principle using rapacuronium and a comparison with rocuronium and mivacurium. After induction, 120 patients were randomly allocated to six similar groups. Groups 1 and 2 received rapacuronium 1000 micrograms.Kg-1 as a bolus or primed with 100 micrograms.Kg-1. To groups 3 and 4, rocuronium 400 micrograms.Kg-1 were given as a bolus or primed with 60 micrograms.Kg-1, finally mivacurium 100 micrograms.Kg-1 was used for groups 5 and 6 by bolus or primed with 10 micrograms.Kg-1. Neuromuscular function was monitored by electromyography and it was demonstrated that time to 80% blockade, is significantly shorter after priming: 137 (bolus) vs 101 seconds (priming) for rapacuronium, 160 vs 90 for rocuronium and 196 vs 118 for mivacurium. Onset time was also statistically accelerated by priming: 229 seconds vs 183, 289 vs 203 and 298 vs 252 respectively. No significant change was noticed in maximal blockade and clinical duration due to priming. During early onset, only the mivacurium patients showed a statistical difference in train of four fade between bolus and priming. In conclusion, priming hasten early and maximal effect produced by rapacuronium, rocuronium and mivacurium without any change in maximal blockade and clinical duration. Pre-synaptic effect does not explain consistently the mode of action of priming.

摘要

本研究的目的是阐述预充原理在罗库溴铵中的药效学,并与罗库溴铵和米库氯铵进行比较。诱导后,120例患者被随机分为六个相似的组。第1组和第2组接受1000微克·千克⁻¹的罗库溴铵静脉推注或先予100微克·千克⁻¹预充。第3组和第4组给予400微克·千克⁻¹的罗库溴铵静脉推注或先予60微克·千克⁻¹预充,最后第5组和第6组给予100微克·千克⁻¹的米库氯铵静脉推注或先予10微克·千克⁻¹预充。采用肌电图监测神经肌肉功能,结果表明预充后达到80%阻滞的时间显著缩短:罗库溴铵静脉推注为137秒,预充为101秒;罗库溴铵静脉推注为160秒,预充为90秒;米库氯铵静脉推注为196秒,预充为118秒。预充也使起效时间在统计学上加快:分别为229秒对183秒、289秒对203秒和298秒对252秒。预充对最大阻滞和临床持续时间无显著影响。在起效早期,只有米库氯铵组患者在单次静脉注射和预充之间的四个成串刺激衰减方面存在统计学差异。总之,预充可加速罗库溴铵、罗库溴铵和米库氯铵产生的早期和最大效应,而最大阻滞和临床持续时间无任何变化。突触前效应并不能始终如一地解释预充的作用方式。

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