首页> 外文期刊>Drug development and industrial pharmacy >Drug dispersion degree and drug dissolution rate in Hybrane S1200-based instant-release matricial particles prepared by hot melt extrusion
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Drug dispersion degree and drug dissolution rate in Hybrane S1200-based instant-release matricial particles prepared by hot melt extrusion

机译:热熔挤出制备的基于Hybrane S1200的速释基质颗粒中的药物分散度和药物溶解率

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摘要

The objective of this study is to evaluate the dissolution of a poorly soluble drug (prednisolone) from different sized matricial particles (from <250 to >1500 mm) with two drug contents (10% or 20%) obtained by hot melt extrusion using the hyperbranched polyesteramide Hybrane S1200 (water-soluble and with a Tg of 45 degrees C) as the carrier. X-ray diffraction, differential scanning calorimetry and SEM studies permit us to conclude that in 10% prednisolone extrudate, the drug is mainly dispersed within the carrier, whereas in those containing 20% an important fraction of the drug remains in a crystalline state and is accumulated on the surface of the extrudates. On particles proceeding from 10% drug extrudate, the drug dissolution rate is very high and slightly dependant on particle size and in all cases, higher than the pure micronized drug. However, on particles proceeding from 20% prednisolone extrudate particle size have a major effect on drug dissolution rate, attributable to higher proportions of crystalline drug accumulated on the surface, hindering polymer dissolution. Thus, the reduction of the particle size after extrudate grinding creates new surfaces from inside, that leads to strong increments on prednisolone dissolution rate, and becomes higher than the pure micronized drug one when the particle size is <250 mu m.
机译:这项研究的目的是评估难溶性药物(泼尼松龙)从不同尺寸的基质颗粒(<250至> 1500 mm)中的溶出度,其中两种药物含量(10%或20%)通过热熔挤出使用超支化聚酯酰胺Hybrane S1200(水溶性,Tg为45摄氏度)作为载体。 X射线衍射,差示扫描量热法和SEM研究使我们得出以下结论:在10%泼尼松龙挤出物中,药物主要分散在载体中,而在含有20%泼尼松龙的药物中,药物的重要部分保持结晶状态,并且积聚在挤出物表面上。在从10%的药物挤出物中产生的颗粒上,药物的溶出率非常高,并且略微取决于粒径,并且在所有情况下均高于纯微粉化的药物。但是,对于从20%泼尼松龙挤出物开始生产的颗粒,其粒径对药物溶出速率有重大影响,这归因于结晶药物在表面上积累的比例更高,从而阻碍了聚合物的溶出。因此,挤出物研磨后粒径的减小从内部产生了新的表面,这导致泼尼松龙溶解速率的强烈增加,并且当粒径<250μm时变得高于纯微粉化药物之一。

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