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采用析因设计对双氯芬酸钠控释微球进行处方优化。

Formulation optimization of controlled release diclofenac sodium microspheres using factorial design.

作者信息

Gohel M C, Amin A F

机构信息

Department of Pharmaceutics and Pharmaceutical Technology, L.M. College of Pharmacy, Navrangpura, Ahmedabad, India.

出版信息

J Control Release. 1998 Feb 12;51(2-3):115-22. doi: 10.1016/s0168-3659(97)00102-8.

Abstract

Diclofenac sodium is an ideal candidate for incorporation in a controlled release device to diminish its adverse effects after oral administration. Microspheres were prepared by using sodium alginate as a polymer and CaCl2 as a cross-linking agent. In this investigation, 3(3) full factorial design was used to investigate the joint influence of the three variables: the stirring speed (X1), concentration of CaCl2 (X2) and % of heavy liquid paraffin in a blend of heavy and light liquid paraffin in the dispersion medium (X3) on the time of 80% drug dissolution (t80). Potential variables such as concentration of sodium alginate and drug: sodium alginate ratio were kept constant in the experimental design. A statistical model with significant interaction terms is derived to predict t80. The results of multiple linear regression analysis and F-statistics revealed that for obtaining controlled drug release, the microspheres should be prepared using relatively lower stirring speed, higher concentration of CaCl2 and higher percentage of heavy liquid paraffin in the dispersion medium. The X1X2 and X2X3 interactions were found to be statistically significant in nature. A response surface plot is presented to show the effects of X1, X2 and X3 on t80. The drug was released by diffusion of anomalous type. A model was validated for accurate prediction of drug release profile. Acceptable batches were identified in the experimental design with constraints on percentage drug released in 1, 6 and 8 h.

摘要

双氯芬酸钠是一种理想的药物,适合制成控释制剂以减少口服后的不良反应。以海藻酸钠为聚合物、氯化钙为交联剂制备微球。在本研究中,采用3(3)全因子设计来研究搅拌速度(X1)、氯化钙浓度(X2)和分散介质中重质与轻质液体石蜡混合物中重质液体石蜡的百分比(X3)这三个变量对80%药物溶解时间(t80)的联合影响。在实验设计中,海藻酸钠浓度和药物与海藻酸钠比例等潜在变量保持恒定。推导了一个具有显著交互项的统计模型来预测t80。多元线性回归分析和F统计结果表明,为实现控释,应采用相对较低的搅拌速度、较高的氯化钙浓度以及分散介质中较高百分比的重质液体石蜡来制备微球。发现X1X2和X2X3交互作用具有统计学显著性。给出了响应面图以显示X1、X2和X3对t80的影响。药物以非规则扩散方式释放。验证了一个模型以准确预测药物释放曲线。在实验设计中确定了可接受的批次,并对1、6和8小时内的药物释放百分比进行了限制。

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