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首页> 外文期刊>European journal of pharmaceutics and biopharmaceutics: official journal of Arbeitsgemeinschaft fuer Pharmazeutische Verfahrenstechnik e.V >Optimised process and formulation conditions for extended release dry polymer powder-coated pellets.
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Optimised process and formulation conditions for extended release dry polymer powder-coated pellets.

机译:优化的工艺和配方条件,用于缓释干燥的聚合物粉末包衣小丸。

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摘要

The objective of this study was to improve the film formation and permeability characteristics of extended release ethylcellulose coatings prepared by dry polymer powder coating for the release of drugs of varying solubility. Ethylcellulose (7 and 10 cp viscosity grades) and Eudragit(R) RS were used for dry powder coating of pellets in a fluidised bed ball coater. Pre-plasticised ethylcellulose powder was prepared by spray-drying aqueous ethylcellulose dispersions (Surelease(R) and Aquacoat(R)) or by hot melt extrusion/cryogenic grinding of plasticised ethylcellulose. Chlorpheniramine maleate and theophylline were used as model drugs of different solubilities. The film formation process, polymeric films and coated pellets were characterised by differential scanning calorimetry (DSC), dynamic mechanical analysis (DMA), scanning electron microscopy (SEM) and dissolution testing. Film formation and extended drug release was achieved with ethylcellulose, a polymer with a high glass transition temperature (T(g)) without the use of water, which is usually required in dry powder coating. DMA-measurements revealed that plasticised ethylcellulose had a modulus of elasticity (E') similar to the low T(g) Eudragit(R) RS. With increasing plasticiser concentration, the T(g) of ethylcellulose was reduced and the mechanical properties improved, thus facilitating coalescence of the polymer particles. SEM-pictures revealed the formation of a dense, homogeneous film. The lower viscosity grade ethylcellulose (7 cp) resulted in better film formation than the higher viscosity grade (10 cp) and required less stringent curing conditions. Successful extended release ethylcellulose coatings were also obtained by coating with pre-plasticised spray-dried ethylcellulose powders as an alternative to the separate application of pure ethylcellulose powder and plasticiser. The permeability of the extended release coating could be controlled by using powder blends of ethylcellulose with the hydrophilic polymer HPMC. In conclusion, dry polymer powder coating is an interesting technique to achieve extended release of drugs with varying solubility as an alternative to classical coatings obtained from organic polymer solution or aqueous polymer dispersions.
机译:这项研究的目的是改善通过干聚合物粉末包衣制备的缓释乙基纤维素包衣的成膜性和渗透性,以释放各种溶解度的药物。乙基纤维素(粘度等级为7和10 cp)和EudragitRS用于在流化床球包衣机中对丸粒进行干粉包衣。通过将乙基纤维素水分散体(Surelease和Aquacoat)喷雾干燥或通过热熔挤出/低温研磨增塑的乙基纤维素来制备预增塑的乙基纤维素粉末。马来酸氯苯那敏和茶碱被用作不同溶解度的模型药物。通过差示扫描量热法(DSC),动态力学分析(DMA),扫描电子显微镜(SEM)和溶出度测试对膜的形成过程,聚合物膜和包衣的颗粒进行了表征。用乙基纤维素可以实现成膜和延长药物释放,乙基纤维素是一种具有高玻璃化转变温度(T(g))的聚合物,而无需用水,这在干粉涂料中通常是必需的。 DMA测量显示增塑的乙基纤维素具有类似于低T(g)RS的弹性模量(E')。随着增塑剂浓度的增加,乙基纤维素的T(g)降低,机械性能提高,从而促进了聚合物颗粒的聚结。 SEM照片显示形成了致密的均匀膜。较低粘度等级的乙基纤维素(7厘泊)比较高粘度等级的10厘泊产生更好的成膜性,并且所需的固化条件更少。通过用预增塑的喷雾干燥的乙基纤维素粉末进行涂层也可以获得成功的缓释乙基纤维素涂层,这是单独使用纯乙基纤维素粉末和增塑剂的替代方法。可以通过使用乙基纤维素与亲水性聚合物HPMC的粉末共混物来控制缓释涂层的渗透性。总之,干粉聚合物粉末涂料是一种有趣的技术,它可以实现溶解度不同的药物的延长释放,以替代从有机聚合物溶液或水性聚合物分散体中获得的经典涂料。

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