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A double-layered gastric floating tablet for zero-order controlled release of dihydromyricetin: Design, development, and in vitro/in vivo evaluation

生物利用度 药理学 药代动力学 药品 体内 药效学 零阶 化学 一级 医学 数学 应用数学 生物 生物技术
作者
Ruirui Zhang,Houyin Shi,Sifang Li,Hao Zhang,Dan Zhang,Ailing Wu,Chun Zhang,Chunhong Li,Xiujuan Fu,Siwei Chen,Jiaoyue Shi,Yang Tian,Sihan Wang,Yu Wang,Hao Liu
出处
期刊:International Journal of Pharmaceutics [Elsevier]
卷期号:638: 122929-122929 被引量:15
标识
DOI:10.1016/j.ijpharm.2023.122929
摘要

Dihydromyricetin (DHM) is an important natural flavonoid. However, most of DHM preparations have shown shortcomings such as low drug loading, poor drug stability, and/or large fluctuations in blood concentration. This study aimed to develop a gastric floating tablet with a double-layered structure for zero-order controlled release of DHM (DHM@GF-DLT). The final product DHM@GF-DLT showed a high average cumulative drug release at 24 h that best fit the zero-order model, and had a good floating ability in the stomach of the rabbit with a gastric retention time of over 24 h. The FTIR, DSC, and XRPD analyses indicated the good compatibility among the drug and the excipients in DHM@GF-DLT. The pharmacokinetic study revealed that DHM@GF-DLT could prolong the retention time of DHM, reduce the fluctuation of blood drug concentration, and enhance the bioavailability of DHM. The pharmacodynamic studies demonstrated that DHM@GF-DLT had a potent and long-term therapeutic effect on systemic inflammation in rabbits. Therefore, DHM@GF-DLT had the potential to serve as a promising anti-inflammatory agent and may develop into a once-a-day preparation, which was favorable to maintain a steady blood drug concentration and a long-term drug efficacy. Our research provided a promising development strategy for DHM and other natural products with a similar structure to DHM for improving their bioavailability and therapeutic effect.
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