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首页> 外文期刊>藥學雜誌 >Preparation, characterization and in vitro dissolution studies of solid dispersion of meloxicam with PEG 6000.
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Preparation, characterization and in vitro dissolution studies of solid dispersion of meloxicam with PEG 6000.

机译:美洛昔康与PEG 6000的固体分散体的制备,表征和体外溶出研究。

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摘要

The poor solubility and wettability of meloxicam leads to poor dissolution and hence showing variations in bioavailability. The present study is aimed to increase solubility and dissolution of the drug using solid dispersion techniques. The solid binary systems were prepared at various drug concentrations (5-40%) with polyethylene glycol 6000 by different techniques (physical mixing, solvent evaporation). The formulations were characterized by solubility studies, differential scanning calorimetry, fourier transform infrared spectroscopy and in vitro dissolution rate studies. The solubility of drug increased linearly with increase in polymer concentration showing A(L) type solubility diagrams. Infrared spectroscopy studies indicated the possibility of hydrogen bonding with polymer. The differential scanning calorimetry and powder X ray diffraction demonstrated the presence of polymer as eutectica or monotectica in solid dispersion along with the physical characteristics of the drug (crystalline, amorphous or a mixture of both). The solid dispersions of the drug demonstrated higher drug dissolution rates than physical mixtures and pure meloxicam, as a result of increased wettability and dispersibility of drug in a solid dispersion system.
机译:美洛昔康的差的溶解度和润湿性导致差的溶出度,因此显示出生物利用度的变化。本研究旨在使用固体分散技术来增加药物的溶解度和溶解度。通过不同的技术(物理混合,溶剂蒸发)用聚乙二醇6000制备了各种药物浓度(5-40%)的固体二元体系。通过溶解度研究,差示扫描量热法,傅立叶变换红外光谱法和体外溶出速率研究来表征制剂。药物的溶解度随聚合物浓度的增加呈线性增加,显示A(L)型溶解度图。红外光谱研究表明氢与聚合物键合的可能性。差示扫描量热法和粉末X射线衍射证明了固体分散体中存在作为共聚或单聚的聚合物以及药物的物理特性(晶体,无定形或两者的混合物)。药物的固体分散体显示出比物理混合物和纯美洛昔康更高的药物溶解速率,这是由于药物在固体分散体系中的润湿性和分散性提高。

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