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首页> 外文期刊>Brazilian Journal of Pharmaceutical Sciences >Preparation and characterization of cefuroxime axetil solid dispersions using poloxamer 188
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Preparation and characterization of cefuroxime axetil solid dispersions using poloxamer 188

机译:使用泊洛沙姆188制备头孢呋辛酯酯固体分散体并进行表征

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摘要

The main objective of the present work was to enhance the solubility and dissolution rate of poorly water-soluble drug cefuroxime axetil (CA) by formulating it into solid dispersions (SDs) with water soluble carrier poloxamer 188. Different methods were employed to prepare the dispersion, such as: Solvent method (SM), Kneading method (KM), Melt evaporation method (MEM) and Physical mixture (PM) in different drug: carrier ratios 1:1, 1:2 and 1:3 (cefuroxime axetil: poloxamer 188). The physical mixture(s) and solid dispersion(s) were characterized for drug carrier interaction, drug content, solubility, dissolution rate, differential scanning calorimetry (DSC) and FT-IR study. The dissolution rate of the prepared solid dispersion systems was determined in phosphate buffer (pH 6.8) for 1 h. The solubility of drug from different systems was also determined in water. All SD formulations were found to have a higher dissolution rate comparatively to pure CA. The dissolution rate was enhanced in the following order SM MEM KM. The enhancement of dissolution rate may be caused by increase wettability, dispersibillity reduction in particle size or the formation of CA β crystalline. The FT-IR study probability revealed that there was no chemical interaction between drug and poloxamer 188.
机译:本工作的主要目的是通过与水溶性载体泊洛沙姆188一起配制为固体分散体(SD),从而提高水溶性差的头孢呋辛酯(CA)的溶解度和溶解速率。采用不同的方法制备分散体,例如:不同药物:载体比例1:1、1:2和1:3(头孢呋辛酯:泊洛沙姆)中的溶剂法(SM),捏合法(KM),熔体蒸发法(MEM)和物理混合物(PM) 188)。对物理混合物和固体分散体进行了药物载体相互作用,药物含量,溶解度,溶出度,差示扫描量热法(DSC)和FT-IR研究的表征。在磷酸盐缓冲液(pH 6.8)中测定制备的固体分散体系统的溶解速率1小时。还测定了来自不同系统的药物在水中的溶解度。发现所有SD制剂相对于纯CA具有更高的溶出速率。溶解速率按以下顺序提高:SM> MEM> KM。溶解速率的提高可能是由于润湿性的提高,粒径分散性的降低或CAβ晶体的形成。 FT-IR研究的可能性表明,药物与泊洛沙姆188之间没有化学相互作用。

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