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甘露醇包衣羟丙基甲基纤维素作为用于对湿度敏感药物的直接压片控释辅料:稳定性视角

Mannitol-Coated Hydroxypropyl Methylcellulose as a Directly Compressible Controlled Release Excipient for Moisture-Sensitive Drugs: A Stability Perspective.

作者信息

Kang Christina Yong Xin, Chow Keat Theng, Lui Yuan Siang, Salome Antoine, Boit Baptiste, Lefevre Philippe, Hiew Tze Ning, Gokhale Rajeev, Heng Paul Wan Sia

机构信息

Roquette Asia Pacific Pte. Ltd., 11 Biopolis Way, Helios, #05-06, Singapore 138667, Singapore.

GEA-NUS Pharmaceutical Processing Research Laboratory, Department of Pharmacy, National University of Singapore, 18 Science Drive 4, Singapore 117543, Singapore.

出版信息

Pharmaceuticals (Basel). 2024 Sep 4;17(9):1167. doi: 10.3390/ph17091167.

Abstract

BACKGROUND/OBJECTIVES: Hydroxypropyl methylcellulose (HPMC) is one of the most commonly used hydrophilic polymers in formulations of matrix tablets for controlled release applications. However, HPMC attracts moisture and poses issues with drug stability in formulations containing moisture-sensitive drugs.

METHODS

Herein, the moisture sorption behavior of excipients and drug stability using aspirin as the model drug in matrix tablets were evaluated, using HPMC and the newly developed mannitol-coated HPMC, under accelerated stability conditions (40 °C, 75% relative humidity) with open and closed dishes.

RESULTS

Tablets prepared with mannitol-coated HPMC showed a slower drug degradation rate compared to tablets prepared with directly compressible HPMC. Initial moisture content and hygroscopicity were stronger predictors of drug stability compared to water activity when comparing samples without similar moisture content. In the early stage (day 0 to 30), the aspirin degradation rate was similar in both open and closed conditions, as moisture content is the main degradation contributor. In the later stage (day 30 to 90), aspirin degradation was faster under closed conditions than under open conditions, likely due to autocatalytic effects caused by the volatile acidic by-product entrapped in the closed environment.

CONCLUSIONS

The findings from this study reinforced the importance of judicious excipient selection based on the understanding of excipient-moisture interactions to maximize the chemical stability of moisture-sensitive drugs. Mannitol-coated HPMC is a promising addition to the formulator's toolbox for the formulation of controlled release dosage forms by direct compression.

摘要

背景/目的:羟丙基甲基纤维素(HPMC)是用于控释制剂的基质片剂配方中最常用的亲水性聚合物之一。然而,HPMC会吸湿,在含有对湿度敏感药物的制剂中会引发药物稳定性问题。

方法

本文以阿司匹林为模型药物,在加速稳定性条件(40℃,75%相对湿度)下,使用开放和封闭培养皿,评估了辅料的吸湿行为以及在基质片剂中药物的稳定性,使用了HPMC和新开发的甘露醇包衣的HPMC。

结果

与直接压片用HPMC制备的片剂相比,用甘露醇包衣的HPMC制备的片剂显示出较慢的药物降解速率。在比较含水量不相似的样品时,初始含水量和吸湿性比水分活度更能预测药物稳定性。在早期阶段(第0天至30天),开放和封闭条件下阿司匹林的降解速率相似,因为含水量是主要的降解因素。在后期阶段(第30天至90天),封闭条件下阿司匹林的降解比开放条件下更快,这可能是由于封闭环境中截留的挥发性酸性副产物引起的自催化作用。

结论

本研究结果强化了基于对辅料-水分相互作用的理解明智选择辅料以最大化对湿度敏感药物化学稳定性的重要性。甘露醇包衣的HPMC是配方设计师用于直接压片制备控释剂型的工具包中有前景的新增材料。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/fc3c/11435371/18406b742c94/pharmaceuticals-17-01167-g001.jpg

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