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载体尺寸和形态对不同流速下硫酸沙丁胺醇雾化后分散情况的影响。

The effects of carrier size and morphology on the dispersion of salbutamol sulphate after aerosolization at different flow rates.

作者信息

Zeng X M, Martin G P, Marriott C, Pritchard J

机构信息

Department of Pharmacy, King's College London, UK.

出版信息

J Pharm Pharmacol. 2000 Oct;52(10):1211-21. doi: 10.1211/0022357001777342.

Abstract

We have investigated the interdependence of various factors (particle size, surface smoothness, carrier particle shape, inhalation flow rate) on the deposition of a model drug (salbutamol sulphate) after aerosolization from a model inhaler device (Rotahaler). Different batches of alpha-lactose monohydrate were prepared to have different particle size, particle shape and surface smoothness. Each batch of lactose was then mixed separately with salbutamol sulphate in a ratio of 67.5 : 1 (w/w), under similar conditions. Drug deposition from each formulation was investigated using a 4-stage liquid impinger after aerosolization at 28.3, 60.0 and 96.0 L min(-1) via a Rotahaler. At a flow rate of 28.3 L min(-1), a large portion of drug particles was not emitted from the inhaler, the % emission varying from 29.6% to 66.6% for all formulations investigated. Drug emission tended to increase with particle size of the carrier whilst fine particle fraction, fine particle dose and dispersibility appeared to increase with decreasing particle size but increasing elongation ratio of the carrier particles. Increasing the flow rate to 60.0 L min(-1) was shown to increase drug emission since > 75% total dose was found to be emitted from the inhaler. Again, smaller or more elongated lactose particles resulted in a higher fine particle dose or fine particle fraction of salbutamol sulphate than the coarser carrier, although they produced a similar (analysis of variance P > 0.05) drug emission. Increasing the flow rate to 96.0 L min(-1) did not increase drug emission. Increasing the flow rate resulted in an increase in the fine particle fraction and fine particle dose of salbutamol sulphate from all formulations. The flow rate of the airstream appeared to play the most important role, followed by particle size and elongation ratio of the carrier particles, with the surface smoothness relatively less significant in determining the deposition of salbutamol sulphate from the Rotahaler.

摘要

我们研究了各种因素(粒径、表面光滑度、载体颗粒形状、吸入流速)对模型药物(硫酸沙丁胺醇)从模型吸入装置(旋转吸入器)雾化后沉积的相互依赖性。制备了不同批次的一水合α-乳糖,使其具有不同的粒径、颗粒形状和表面光滑度。然后,在相似条件下,将每批乳糖分别与硫酸沙丁胺醇按67.5:1(w/w)的比例混合。使用四阶段液体冲击器,在通过旋转吸入器以28.3、60.0和96.0 L min⁻¹的流速雾化后,研究每种制剂的药物沉积情况。在流速为28.3 L min⁻¹时,大部分药物颗粒未从吸入器中喷出,所有研究制剂的喷出百分比在29.6%至66.6%之间变化。药物喷出量倾向于随载体粒径的增加而增加,而细颗粒分数、细颗粒剂量和分散性似乎随粒径减小但载体颗粒伸长率增加而增加。将流速提高到60.0 L min⁻¹可增加药物喷出量,因为发现吸入器喷出的总剂量超过75%。同样,较小或更细长的乳糖颗粒比较粗的载体产生的硫酸沙丁胺醇细颗粒剂量或细颗粒分数更高,尽管它们产生的药物喷出量相似(方差分析P>0.05)。将流速提高到96.0 L min⁻¹并没有增加药物喷出量。流速增加导致所有制剂中硫酸沙丁胺醇的细颗粒分数和细颗粒剂量增加。气流流速似乎起着最重要的作用,其次是载体颗粒的粒径和伸长率,表面光滑度在决定旋转吸入器中硫酸沙丁胺醇的沉积方面相对不太重要。

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