杆菌肽锌负载 pla 复合材料释放动力学行为模型和保质期评估的比较研究

A. Özarslan, Fatih Ciftci
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引用次数: 0

摘要

建立数学模型的目的是简化复杂的药物释放过程,了解特定材料系统的释放机制。因此,数学模型主要关注一到两个重要因素。药物释放的目的是最大限度地提高天然衍生和合成大分子的生物活性,从而提高其临床适用性并改善整体生活质量。本研究的重点是制备含有不同重量百分比(0.5、1.0 和 2.0)的杆菌肽锌聚乳酸复合材料,并评估其作为药物释放系统的潜力。为了解巴曲锌从聚乳酸复合材料中的释放机制,我们建立了弗兰兹扩散动力学模型和累积释放动力学数学模型。利用弗兰兹扩散模型分析了聚乳酸/杆菌肽锌复合结构的释放行为。结果表明,该结构具有持续的释放速率,遵循零阶释放动力学模式。此外,复合结构的保质期被确定为 125 天。为了比较不同重量百分比的释放行为和保质期,我们采用 Python 程序设计来模拟释放行为,并估算出加入聚乳酸基质中的杆菌肽锌(0.5、1.0 和 2.0)的保质期。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
A COMPARATIVE STUDY OF RELEASE KINETICS BEHAVIOR MODELS AND SHELF LIFE ASSESSMENT OF BACITRACIN ZINC-LOADED PLA COMPOSITES
Mathematical modeling aims to simplify the complex process of drug release and to gain knowledge about the release mechanisms specific to a given material system. Consequently, a mathematical model focuses primarily on one or two important factors. Drug release aims to maximize the bioactivity of both naturally derived and synthetically derived macromolecules, thus increasing their clinical applicability and improving the overall quality of life. This study focused on fabricating PLA composites with different weight percentages of Bacitracin Zinc (0.5, 1.0, and 2.0) and evaluating their potential as a drug delivery system. To understand the release mechanism of Bacitracin Zinc from the PLA composites, we developed a Franz diffusion kinetic model and a mathematical model for cumulative release kinetics. The Franz diffusion model was utilized to analyze the release behavior of the PLA/Bacitracin Zinc composite structure. The results indicated a sustained release rate, following a Zero Order release kinetics pattern. Furthermore, the shelf life of the composite structure was determined to be 125 days. Python programming was employed to model the release behavior and estimate the shelf life of Bacitracin Zinc (0.5, 1.0, and 2.0) incorporated into the PLA matrix to compare different weight percentages' behavior and shelf life.
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