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Effect of multiple actuations, delayed inhalation and antistatic treatment on the lung bioavailability of salbutamol via a spacer device.

机译:通过间隔装置多次驱动,延迟吸入和抗静电治疗对沙丁胺醇肺部生物利用度的影响。

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摘要

BACKGROUND: The aim of this study was to extend previous in vitro observations regarding the effects of multiple actuations of aerosols into spacer devices, delayed inhalation, and antistatic treatment of spacer devices on the amount of drug delivered for inhalation. An in vivo study of lung bioavailability of salbutamol from a large volume (Volumatic) spacer was conducted. METHODS: Ten healthy volunteers of mean age 20.5 years with a mean forced expiratory volume in one second of 112.1% predicted were studied in a randomised single blind (investigator blind) crossover study. 1200 micrograms of salbutamol was given with mouth rinsing (100 micrograms/puff) on four study days: single puffs via spacer, multiple puffs via spacer (3 x 4 puffs), single puffs with 20 second delay before inhalation via spacer, and single puffs via an antistatic treated spacer. All spacers, including those treated with antistatic, were prewashed prior to each study day. Measurements of lung bioavailability were made at five, 10, and 20 minutes after inhalation to determine peak (Cmax) and average (Cav) plasma salbutamol levels. Systemic beta 2 responses including finger tremor, heart rate, and plasma potassium levels were also evaluated. RESULTS: Single puffs from the spacer produced higher plasma salbutamol levels and greater systemic beta 2 responses than either multiple puffs or single puffs with delayed inhalation for a 1200 micrograms dose. For Cmax this amounted to a 1.93-fold (95% CI 1.68 to 2.19) greater lung bioavailability for single puffs than for multiple puffs and a 1.80-fold (95% CI 1.59 to 2.00) greater lung bioavailability for single puffs than for single puffs with a 20 second delay. Comparison of the normal and antistatic treated spacers (both prewashed) revealed differences for Cmax with levels 1.23-fold (95% CI 1.04 to 1.41) greater for the normal spacer. CONCLUSIONS: Delayed inhalation from a Volumatic spacer and the use of multiple puffs results in a considerable decrease in the delivery of salbutamol to the lungs with an approximate twofold reduction in lung bioavailability. Washing a Volumatic spacer is as effective as an antistatic lining in reducing the effects of static charge on salbutamol delivery in vivo.
机译:背景:这项研究的目的是扩展先前对气雾剂多次致动间隔装置,延迟吸入以及间隔装置的抗静电处理对吸入的药物量的影响的体外观察。进行了从大体积(体积)间隔物中沙丁胺醇在肺部生物利用度的体内研究。方法:在一项随机单盲(研究盲)交叉研究中,研究了10名平均年龄20.5岁,平均强迫呼气量为12.1%的健康志愿者。在四个研究日内用漱口水给予1200微克沙丁胺醇(100微克/粉扑):通过隔垫单口抽吸,通过隔垫单口抽吸(3 x 4抽吸),通过隔垫吸入前延迟20秒的单口抽吸和单口抽吸通过抗静电处理的垫片。在每个研究日之前,将所有垫片(包括用抗静电剂处理过的垫片)预先清洗。在吸入后五,十和二十分钟进行肺生物利用度的测定,以确定血浆沙丁胺醇的峰值(Cmax)和平均(Cav)水平。还评估了系统性β2反应,包括手指震颤,心律和血浆钾水平。结果:与1200毫克剂量的多次抽吸或单次抽吸延迟吸入相比,间隔器单次抽吸可产生更高的血浆沙丁胺醇水平和更大的系统性β2反应。对于Cmax,单口抽吸的肺生物利用度比单口抽吸高1.93倍(95%CI为1.68至2.19),比单口抽吸肺生物利用度高1.93倍(95%CI为1.59至2.00)。延迟20秒正常垫片和抗静电垫片的比较(均已预洗)表明,Cmax的差异为正常垫片的1.23倍(95%CI 1.04至1.41)。结论:从Volumatic垫片中延迟吸入和使用多次抽吸会导致沙丁胺醇向肺部的输送显着减少,并且肺生物利用度降低大约两倍。洗涤Volumatic间隔物与抗静电衬里一样有效,可减少静电荷对体内沙丁胺醇释放的影响。

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