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首页> 外文期刊>Acta Chimica Slovenica >QbD Based Approach to Enhance the In- Vivo Bioavailability of Ethinyl Estradiol in Sprague- Dawley Rats
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QbD Based Approach to Enhance the In- Vivo Bioavailability of Ethinyl Estradiol in Sprague- Dawley Rats

机译:基于QBD基于QBD的方法,提高了乙炔雌二醇在Sprague-Dawley大鼠中的体内生物利用度

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Lyophilized nanosuspension of poorly soluble Ethinyl estradiol (EE) was fabricated to enhance its solubility and bioavailability using a quality-by-design (QbD) approach. With the help of the Ishikawa diagram, prospective risk factors were identified and screened by Placket–Burman design to investigate the effects of formulation and process variables on dependent variables. The number of cycles (X4), the concentration of soya lecithin (X5) and the concentration of tween 80 (X7) were identified as significant factors (P0.05), which were further optimized using Central Composite Design. The mean particle size, zeta potential, drug content and entrapment efficiency of optimized lyophilized EE nanosuspension (EENPs) was 220±0.37 nm, -19.3±6.73 mV, 92.23±0.45%, 99.52±0.52%, respectively. Significantly, EENPs enhances C max and AUC 0-t by 1.5, 1.7 folds and relative bioavailability by 2-fold with its distribution being at higher concentrations in the liver, spleen, and stomach. Thus, QbD based approach for the development of nanosuspension could be an absolute, optimistic approach to identify the critical process parameters and critical quality attributes.
机译:制备冻干含乙醇溶解乙醇(EE)的冻干纳米悬浮剂,以增强其使用质量 - 设计质量(QBD)方法的溶解度和生物利用度。在Ishikawa图的帮助下,通过Placket-Burman设计确定并筛查了预期风险因素,以研究对依赖变量的制剂和过程变量的影响。循环(X4),大豆卵磷脂浓度(X5)的浓度和吐温80(X7)的浓度被鉴定为显着因子(P <0.05),使用中央复合设计进一步优化。优化的冻干EE纳米术(EENPS)的平均粒度,ζ电位,药物含量和夹带效率为220±0.37nm,-19.3±6.73mV,92.23±0.45%,99.52±0.52%。值得注意的是,Eenps通过2倍的分布在肝脏,脾胃和胃中处于较高浓度的情况下,EENPS增强了1.5,1.7折叠和相对生物利用度。因此,基于QBD的纳米柱术的方法可以是绝对的乐观方法来识别临界过程参数和关键质量属性。

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