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精细辅料在载药干粉吸入剂混合物中的新作用:混合过程中药物颗粒解团聚作用的揭示。

A New Role of Fine Excipient Materials in Carrier-Based Dry Powder Inhalation Mixtures: Effect on Deagglomeration of Drug Particles During Mixing Revealed.

机构信息

European Egyptian Pharmaceutical Industries, Alexandria,, Egypt.

Department of Pharmaceutics, College of Pharmacy, University of Hail, P.O. Box 6166, Hail, 81442, Saudi Arabia.

出版信息

AAPS PharmSciTech. 2017 Nov;18(8):2862-2870. doi: 10.1208/s12249-017-0767-4. Epub 2017 Apr 18.

Abstract

The potential of fine excipient materials to improve the performance of carrier-based dry powder inhalation mixtures is well acknowledged. The mechanisms underlying this potential are, however, open to question till date. Elaborate understanding of these mechanisms is a requisite for rational rather than empirical development of ternary dry powder inhalation mixtures. While effects of fine excipient materials on drug adhesion to and detachment from surfaces of carrier particle have been extensively investigated, effects on other processes, such as carrier-drug mixing, capsule/blister/device filling, or aerosolization in inhaler devices, have received little attention. We investigated the influence of fine excipient materials on the outcome of the carrier-drug mixing process. We studied the dispersibility of micronized fluticasone propionate particles after mixing with α-lactose monohydrate blends comprising different fine particle concentrations. Increasing the fine (D < 10.0 μm) excipient fraction from 1.84 to 8.70% v/v increased the respirable drug fraction in the excipient-drug mixture from 56.42 to 67.80% v/v (p < 0.05). The results suggest that low concentrations of fine excipient particles bind to active sites on and fill deep crevices in coarse carrier particles. As the concentration of fine excipient particles increases beyond that saturating active sites, they fill the spaces between and adhere to the surfaces of coarse carrier particles, creating projections and micropores. They thereby promote deagglomeration of drug particles during carrier-drug mixing. The findings pave the way for a comprehensive understanding of contributions of fine excipient materials to the performance of carrier-based dry powder inhalation mixtures.

摘要

精细赋形剂材料改善载药干粉吸入剂混合物性能的潜力已得到充分认可。然而,这些潜力的潜在机制至今仍存在争议。详细了解这些机制是实现基于理性而非经验开发三元干粉吸入剂混合物的必要条件。虽然精细赋形剂材料对药物在载体颗粒表面的附着和脱落的影响已经得到了广泛的研究,但对其他过程的影响,如载体-药物混合、胶囊/泡罩/装置填充或吸入装置中的气溶胶化,却很少受到关注。我们研究了精细赋形剂材料对载体-药物混合过程结果的影响。我们研究了在与包含不同精细颗粒浓度的α-乳糖一水合物混合物混合后,微米化丙酸氟替卡松颗粒的分散性。精细(D<10.0μm)赋形剂分数从 1.84%增加到 8.70%(体积比),可使赋形剂-药物混合物中可吸入药物的比例从 56.42%增加到 67.80%(p<0.05)。结果表明,低浓度的精细赋形剂颗粒结合到粗载体颗粒的活性位上并填充其深裂缝。随着精细赋形剂颗粒浓度超过饱和活性位的浓度,它们填充粗载体颗粒之间的空间并附着在其表面,形成突起和微孔。从而在载体-药物混合过程中促进药物颗粒的解聚。这些发现为全面了解精细赋形剂材料对载药干粉吸入剂混合物性能的贡献铺平了道路。

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