Ana S. Sousa, J. Serra, C. Estevens, R. Costa, António J. Ribeiro
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Abstract
Although the development of extended release (ER) matrices has been extensively investigated, understanding the most appropriate mechanism of drug release to achieve the desired release remains a cost- and time-consuming challenge in the early stages of formulation development. This study aimed to investigate the early stage of developing ER hydrophilic matrix tablets containing mirabegron as a model drug, focusing on the effects of polymer type, diluent type, and polymer amount on critical quality attributes (CQAs), namely, tablet swelling and erosion behavior. A full factorial design was employed to explore the interactions of control factors through multivariate regression analysis, emphasizing the application of quality by design (QbD) principles. The swelling and erosion performances of 72 formulations were evaluated. The swelling data were fitted to the Vergnaud model. Finally, in vitro drug release profiles were investigated for four of the formulations studied. The polymer type, diluent type, and polymer amount had distinct effects on the swelling and erosion behavior of the ER matrix tablets. Compared with those with isomalt (G720) or dextrate (DXT), formulations with polyethylene glycol 8000 (P8000) consistently exhibited greater swelling. Additionally, higher molecular weight was correlated with increased swelling within the same polymer type. Hydroxypropylmethylcellulose (HPMC) and polyethylene oxide (PEO)-based formulations showed higher swelling rates, while polyvinyl alcohol (PVA-80) displayed the highest erosion percentage. The findings highlight the significance of incorporating early-stage screening designs to maximize efficiency and optimize time and resource. This approach enables the development of a comprehensive understanding of drug release mechanisms from ER matrix tablets.
尽管对缓释(ER)基质的开发进行了广泛的研究,但在制剂开发的早期阶段,了解最合适的药物释放机制以实现理想的释放效果仍然是一项耗费成本和时间的挑战。本研究旨在调查以米拉贝琼为模型药物的ER亲水基质片剂开发的早期阶段,重点研究聚合物类型、稀释剂类型和聚合物用量对关键质量属性(CQA),即片剂溶胀和侵蚀行为的影响。研究采用了全因子设计,通过多元回归分析探讨了控制因素之间的相互作用,强调了质量源于设计(QbD)原则的应用。对 72 种制剂的溶胀和侵蚀性能进行了评估。膨胀数据与 Vergnaud 模型进行了拟合。最后,对四种配方的体外药物释放曲线进行了研究。聚合物类型、稀释剂类型和聚合物量对 ER 基质片剂的溶胀和侵蚀行为有明显的影响。与含有异麦芽酮(G720)或糊精(DXT)的制剂相比,含有聚乙二醇 8000(P8000)的制剂始终表现出更大的膨胀性。此外,在同一聚合物类型中,分子量越高,膨胀性越大。基于羟丙基甲基纤维素(HPMC)和聚环氧乙烷(PEO)的配方显示出更高的膨胀率,而聚乙烯醇(PVA-80)则显示出最高的侵蚀率。研究结果凸显了采用早期筛选设计以最大限度地提高效率并优化时间和资源的重要性。这种方法有助于全面了解 ER 基质片剂的药物释放机制。
期刊介绍:
AAPS PharmSciTech is a peer-reviewed, online-only journal committed to serving those pharmaceutical scientists and engineers interested in the research, development, and evaluation of pharmaceutical dosage forms and delivery systems, including drugs derived from biotechnology and the manufacturing science pertaining to the commercialization of such dosage forms. Because of its electronic nature, AAPS PharmSciTech aspires to utilize evolving electronic technology to enable faster and diverse mechanisms of information delivery to its readership. Submission of uninvited expert reviews and research articles are welcomed.
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