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载体微观结构在基于粘合剂/载体的干粉吸入混合物中的作用洞察:载体孔隙率和细颗粒含量。

Insights into the roles of carrier microstructure in adhesive/carrier-based dry powder inhalation mixtures: Carrier porosity and fine particle content.

作者信息

Shalash Ahmed O, Molokhia Abdulla M, Elsayed Mustafa M A

机构信息

European Egyptian Pharmaceutical Industries, Alexandria, Egypt.

Department of Pharmaceutics, Faculty of Pharmacy, Alexandria University, Alexandria, Egypt.

出版信息

Eur J Pharm Biopharm. 2015 Oct;96:291-303. doi: 10.1016/j.ejpb.2015.08.006. Epub 2015 Aug 11.

Abstract

To gain insights into complex interactions in carrier-based dry powder inhalation mixtures, we studied the relationships between the carrier microstructural characteristics and performance. We used mercury intrusion porosimetry to measure the microstructural characteristics and to also derive the air permeability of eight carriers. We evaluated the performances of inhalation mixtures of each of these carriers and fluticasone propionate after aerosolization from an Aerolizer®. We did not observe a simple relationship between the carrier total porosity and the performance. Classification of the porosity according to pore size, however, provided interesting insights. The carrier nanoporosity, which refers to pores smaller than micronized drug particles, has a positive influence on the performance. Nanopores reduce the carrier effective contact area and the magnitude of interparticulate adhesion forces in inhalation mixtures. The carrier microporosity, which refers to pores similar in size to drug particles, also has a positive influence on the performance. During mixing, micropores increase the effectiveness of frictional and press-on forces, which are responsible for breaking up of cohesive drug agglomerates and for distribution of drug particles over the carrier surface. On the other hand, the carrier macroporosity, which refers to pores larger than drug particles, apparently has a negative influence on the performance. This influence is likely mediated via the effects of macropores on the powder bed tensile strength and fluidization behavior. The air permeability better represents these effects. The inhalation mixture performance improved as the carrier air permeability decreased. Interestingly, as the carrier fine particle content increased, the carrier microporosity increased and the carrier air permeability decreased. This proposes a new mechanism for the positive effect of fine excipient materials on the performance of carrier-based inhalation mixtures. Fine excipient materials apparently adhere to the surface of coarse carrier particles creating projections and micropores, which increase the effectiveness of mixing. The data also support the mechanism of powder fluidization enforcement by fine excipient materials. The current study clearly demonstrates that the microporosity and the air permeability are key dry powder inhalation carrier performance determinants. Mercury intrusion porosimetry is a useful tool in the dry powder inhalation field; it successfully allowed resolution of carrier pores which contribute differently to the performance.

摘要

为深入了解基于载体的干粉吸入混合物中的复杂相互作用,我们研究了载体微观结构特征与性能之间的关系。我们使用压汞法测量了八种载体的微观结构特征,并推导其透气率。我们评估了这些载体与丙酸氟替卡松各自的吸入混合物经Aerolizer®雾化后的性能。我们未观察到载体总孔隙率与性能之间存在简单关系。然而,根据孔径对孔隙率进行分类提供了有趣的见解。载体纳米孔隙率是指小于微粉化药物颗粒的孔隙,对性能有积极影响。纳米孔减少了载体有效接触面积以及吸入混合物中颗粒间粘附力的大小。载体微孔率是指与药物颗粒大小相似的孔隙,对性能也有积极影响。在混合过程中,微孔增加了摩擦力和压力的作用效果,这些力有助于破碎粘性药物团聚物并使药物颗粒分布在载体表面。另一方面,载体大孔隙率是指大于药物颗粒的孔隙,显然对性能有负面影响。这种影响可能是通过大孔对粉末床抗张强度和流化行为的作用介导的。透气率能更好地体现这些影响。随着载体透气率降低,吸入混合物性能提高。有趣的是,随着载体细颗粒含量增加,载体微孔率增加而载体透气率降低。这提出了一种新机制,解释了细赋形剂材料对基于载体的吸入混合物性能产生积极影响的原因。细赋形剂材料显然附着在粗载体颗粒表面形成凸起和微孔,从而提高了混合效果。数据还支持细赋形剂材料增强粉末流化的机制。当前研究清楚地表明,微孔率和透气率是干粉吸入载体性能的关键决定因素。压汞法是干粉吸入领域的一种有用工具;它成功地解析了对性能有不同贡献的载体孔隙。

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