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Nanoparticle preparation of active pharmaceutical ingredients (APIs) by emulsion solvent diffusion method with cyclodextrins

机译:用环糊精的乳液溶剂扩散法制备活性药物成分(API)的纳米粒子制备

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The objective of the present work is to prepare nanocrystals of APIs using emulsion solvent diffusion method in the existence of cyclodextrin, and to evaluate the effect of cyclodextrin on the particle formation process.A stable crystalline form of indomethacin (IMC) was used as a model drug substance. Several types of cyclodextrin (CyD) solutions, e.g., α-, Β-,γ-CyD solutions, are used as a candidate for outer phase solution. IMC nanoparticles were prepared by the emulsion solvent diffusion method established by Kawashima et al.1) The ethanol solution containing IMC was added into 100 ml of aqueous CyD solution (0.1-1.0 %, w/w) in a 100 mL glass flask using a peristaltic pump at a flow rate of 2.5 mL/min while continuously stirring at 400 rpm with a propeller mixer. The aqueous dispersion was freeze-dried in a vacuum to obtain powdered particles. Freeze dried samples were then dispersed into an aqueous solution to estimate their redispersibility.IMC crystals with a mean diameter of ca. 400 nm were produced by the crystallization process. The freeze dried sample showed porous and braided structure on SEM photograph. These crystals were found to be a methastable form of IMC by using X-ray diffractometry and differential scanning caloriemetry. The freeze dried sample was well dispersed into an aqueous solution as nanocrystals. Although it is well known that CyDs have an ability to form inclusion complexes with a variety of organic compounds due to their peculiar structure, we could not find any evidence for the inclusion complex formation on this method. Interestingly, the nanoparticles of IMC could be formed regardless of types of CyDs used. These results suggest that CyDs in the outer phase suppress the crystal growth and/or aggregation during the emulsion solvent diffusion process, leading to formation of nanosized crystals of IMC in the aqueous solution.
机译:本作工作的目的是使用乳液溶剂扩散法制备API的纳米晶体在存在环糊精中,并评估环糊精对颗粒形成过程的作用。使用稳定的结晶形式的吲哚美辛(IMC)作为模型药物。几种类型的环糊精(CYD)溶液,例如α-,β-,γ-CYD溶液用作外相溶液的候选物。通过Kawashima等Al.1所建立的乳液溶剂扩散方法制备IMC纳米颗粒。使用A的100ml玻璃瓶中的含有IMC的乙醇溶液加入100ml水溶液(0.1-1.0%,w / w)中的100ml玻璃瓶中蠕动泵以2.5ml / min的流速,同时用螺旋桨混合器在400rpm下连续搅拌。在真空中冷冻干燥水分散体,得到粉末状颗粒。将冷冻干燥的样品分散到水溶液中以估计其具有平均直径的可重新分散性。通过结晶过程产生400nm。冷冻干燥的样品在SEM照片上显示多孔和编织结构。通过使用X射线衍射法和差示扫描热量测定,发现这些晶体是IMC的甲型形式的IMC。将冷冻干燥的样品很好地分散到水溶液中作为纳米晶体。众所周知,CYD具有由于其特殊结构而具有各种有机化合物形成包合物复合物的能力,我们无法找到该方法上包含复杂形成的任何证据。有趣的是,无论使用的类型的CYD,也可以形成IMC的纳米颗粒。这些结果表明,外阶段中的树脂在乳液溶剂扩散过程中抑制了晶体生长和/或聚集,导致在水溶液中形成IMC的纳米晶体。

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