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首页> 外文期刊>Pharmaceutical research >Intact nanoparticulate indomethacin in fast-dissolving carrier particles by combined wet milling and aerosol flow reactor methods.
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Intact nanoparticulate indomethacin in fast-dissolving carrier particles by combined wet milling and aerosol flow reactor methods.

机译:通过湿磨和气溶胶流动反应器方法相结合,在快速溶解的载体颗粒中形成完整的纳米颗粒消炎痛。

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摘要

PURPOSE: Drug development is often hindered by a drug's low dissolution rate. We present a method to increase dissolution rate of a drug powder by producing crystalline nanoparticles that are dispersed in carrier microparticles. METHODS: Indomethacin crystals of a few hundred nanometers are prepared by media milling using poloxamer 188 as a stabilizer. Nanoparticles are embedded into microparticles with a mannitol matrix and an L-leucine coating layer using an aerosol flow reactor method. RESULTS: Microparticles stabilize the primary nanoparticles in an intact crystalline form and release them when re-dispersed in aqueous medium. Secondary microparticle structure dissolves rapidly, resulting in a fast release and dissolution of indomethacin. In this manner, it is possible to change the surface layer of the particles from the one needed for nanoparticle production to one more suitable for process formulation of pharmaceuticals for, e.g., tablet or pulmonary products. CONCLUSIONS: Particle assemblies where nano-sized crystalline drug domains are embedded in solid microparticles are presented. The present work is a promising approach towards a "nanos-in-micros" concept as a tool for pharmaceutical nanoparticle processing.
机译:目的:药物的低溶出度通常会阻碍药物的开发。我们提出了一种通过产生分散在载体微粒中的结晶纳米颗粒来提高药物粉末溶解速率的方法。方法:使用泊洛沙姆188作为稳定剂,通过介质研磨制备数百纳米的消炎痛晶体。使用气溶胶流动反应器方法将纳米颗粒嵌入具有甘露醇基质和L-亮氨酸涂层的微粒中。结果:微粒以完整的晶体形式稳定了主要的纳米颗粒,并在重新分散在水性介质中时释放出来。二级微粒结构快速溶解,导致消炎痛快速释放和溶解。以这种方式,可以将颗粒的表面层从生产纳米颗粒所需的表面层改变为更适合用于例如片剂或肺产品的药物的工艺制剂的表面层。结论:提出了在纳米颗粒中嵌入了纳米级药物结构域的颗粒组装体。目前的工作是一种有前景的方法,可将“纳米微颗粒”概念用作药物纳米颗粒加工的工具。

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