一种加压计量吸入器的计算分析和一种新的药物气雾剂靶向方法。

Clement Kleinstreuer, Huawei Shi, Zhe Zhang
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引用次数: 99

摘要

常用的加压计量吸入器(pMDI),特别是用于哮喘治疗,在推进剂的使用和阀门设计方面经历了各种变化。最重要的是选择氢氟烷烃-134a (HFA-134a)作为新的推进剂(而不是氟氯化碳),较小的出口喷嘴直径和附加间隔器,以便最终减小液滴大小和喷雾吸入速度,两者都有助于提高沉积效率,从而更好地治疗哮喘。虽然哮喘病药物相当便宜,但由于pMDI性能不佳引发的全身性副作用,以及这类设备越来越多的使用,以及针对各种肺部和其他疾病的新型靶向药物气溶胶输送,使得详细的性能分析势在必行。考虑到不同的推进剂、喷嘴直径和间隔片的使用,实验验证的计算流体-颗粒动力学技术首次被应用于模拟附着在人体上呼吸道模型上的pMDI中的气流、液滴喷雾传输和气溶胶沉积。结果表明,使用HFA(代替CFC),较小的阀口(0.25 mm代替0.5 mm)和间隔器(ID = 4.2 cm)可以获得最佳性能,主要是因为产生的液滴更小,更容易渗透到支气管气道中。经实验验证的计算机模拟预测,HFA-pMDI和CFC-pMDI的吸入液滴可能分别有46.6%和23.2%到达肺部,两者的喷嘴出口直径均为0.25 mm。常用的吸入器是无方向性的,最多只能实现局部药物气溶胶沉积。然而,当吸入昂贵且积极的药物时,或者必须到达关键的肺部区域时,局部靶向药物气溶胶递送是必不可少的。因此,引入了未来“智能吸入器”系列的基本原理。具体来说,通过产生受控的空气颗粒流,大多数吸入的药物气溶胶到达预定的肺部部位,这些部位与特定疾病和/或治疗有关。使用相同的人类上呼吸道模型,实验证实了从口腔到第3代的受控粒子传输的计算机预测。
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Computational analyses of a pressurized metered dose inhaler and a new drug-aerosol targeting methodology.

The popular pressurized metered dose inhaler (pMDI), especially for asthma treatment, has undergone various changes in terms of propellant use and valve design. Most significant are the choice of hydrofluoroalkane-134a (HFA-134a) as a new propellant (rather than chlorofluorocarbon, CFC), a smaller exit nozzle diameter and attachment of a spacer in order to reduce ultimately droplet size and spray inhalation speed, both contributing to higher deposition efficiencies and hence better asthma therapy. Although asthma medicine is rather inexpensive, the specter of systemic side effects triggered by inefficient pMDI performance and the increasing use of such devices as well as new targeted drug-aerosol delivery for various lung and other diseases make detailed performance analyses imperative. For the first time, experimentally validated computational fluid-particle dynamics technique has been applied to simulate airflow, droplet spray transport and aerosol deposition in a pMDI attached to a human upper airway model, considering different device propellants, nozzle diameters, and spacer use. The results indicate that the use of HFA (replacing CFC), smaller valve orifices (0.25 mm instead of 0.5 mm) and spacers (ID = 4.2 cm) leads to best performance mainly because of smaller droplets generated, which penetrate more readily into the bronchial airways. Experimentally validated computer simulations predict that 46.6% of the inhaled droplets may reach the lung for an HFA-pMDI and 23.2% for a CFC-pMDI, both with a nozzle-exit diameter of 0.25 mm. Commonly used inhalers are nondirectional, and at best only regional drug-aerosol deposition can be achieved. However, when inhaling expensive and aggressive medicine, or critical lung areas have to be reached, locally targeted drug-aerosol delivery is imperative. For that reason the underlying principle of a future line of "smart inhalers" is introduced. Specifically, by generating a controlled air-particle stream, most of the inhaled drug aerosols reach predetermined lung sites, which are associated with specific diseases and/or treatments. Using the same human upper airway model, experimentally confirmed computer predictions of controlled particle transport from mouth to generation 3 are provided.

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