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分形结构决定了整体式渗透泵片的控制释放动力学。

Fractal structure determines controlled release kinetics of monolithic osmotic pump tablets.

机构信息

Center for Drug Delivery System, Shanghai Institute of Materia Medica, Shanghai, 201203, China.

出版信息

J Pharm Pharmacol. 2013 Jul;65(7):953-9. doi: 10.1111/jphp.12056. Epub 2013 Mar 14.

Abstract

OBJECTIVES

To calculate the fractal dimension values of felodipine osmotic pump tablets during drug dissolution and to characterize the mechanism of the controlled drug release kinetics through three-dimensional fractal data.

METHODS

Three-dimensional fractal values of volume (Df,volume ) and surface (Df,surface ) of the tablet core were calculated based on the box counting method.

KEY FINDINGS

During the process of release of felodipine, both Df,volume and Df,surface were within the range of 2-3 and then changed markedly after a period of 3.0 h release, corresponding to extensive changes in entire shape, interior porous channels and surface structure of the tablet core. The curve of Df,volume mirrored that for tablet volume, however the curve of Df,surface was quite different from that of the surface area. Results showed that values of Df,surface correlated well with the drug release rate. Df,surface was found to be an efficient fractal parameter that could be used to characterize the complex changes to the tablet core that take place during drug release.

CONCLUSIONS

The fractal dimension can be used as a quantitative indicator reflecting the drug release performance and be regarded as a key indicator for the quality control of oral controlled drug delivery systems.

摘要

目的

计算非洛地平渗透泵片在药物溶出过程中的分形维数值,并通过三维分形数据来描述控制药物释放动力学的机制。

方法

基于盒计数法计算片剂核心的体积(Df,volume)和表面(Df,surface)的三维分形值。

主要发现

在非洛地平释放过程中,Df,volume 和 Df,surface 均处于 2-3 范围内,然后在 3.0 小时释放后发生明显变化,对应于片剂核心整体形状、内部多孔通道和表面结构的广泛变化。Df,volume 的曲线反映了片剂体积的曲线,而 Df,surface 的曲线与表面积的曲线有很大的不同。结果表明,Df,surface 值与药物释放速率相关性良好。发现 Df,surface 是一个有效的分形参数,可用于描述药物释放过程中片剂核心发生的复杂变化。

结论

分形维数可用作反映药物释放性能的定量指标,并可作为口服控释给药系统质量控制的关键指标。

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