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Development of a furosemide-containing expandable system for gastric retention

速尿 肿胀 的 体内 药理学 溶解试验 化学 医学 生物医学工程 药品 内科学 病理 生物技术 生物 生物制药分类系统
作者
Marco Neumann,Claudia Heimhardt,Knut Seidlitz,Mirko Koziolek,Felix Schneider,Christiane Schiller,Ulrike Hanke,Maria Anschütz,Christian Knopke,Frank Donath,Rudy Thoma,Christian Brätter,Barbara Schug,Hanshermann Franke,Werner Weitschies
出处
期刊:Journal of Controlled Release [Elsevier]
卷期号:338: 105-118 被引量:11
标识
DOI:10.1016/j.jconrel.2021.08.026
摘要

Abstract More than 50 years ago, the first gastroretentive dosage forms came up. Since then, no practical and at the same time reliable gastroretentive system is available on market. A major obstacle in the development of novel gastroretentive systems is the lack of proper predictive test methods. In the present work, we aimed at developing and fully characterizing an expandable gastroretentive system containing furosemide as model drug. On the one hand, we used well-established in vitro tests for drug dissolution and gastroretentive properties (paddle apparatus, swelling characteristics). On the other hand, we used two novel models (dissolution stress test device, mechanical antrum model) to assess these properties under biorelevant conditions. Moreover, we performed an in vivo study under fed and fasted conditions that combined blood sampling and a high-resolution imaging technique (magnetic marker monitoring) to determine gastrointestinal location with the assessment of a pharmacodynamic endpoint (urinary sodium excretion). In vitro dissolution tests confirmed prolonged drug release over more than 8 h independent from pH and with slight pressure sensitivity. Swelling studies indicated good swelling behavior within 4 h along with medium gastroretentive properties as determined with the mechanical antrum model. In vivo imaging showed prolonged gastric residence time after fed compared to fasted administration (481 min vs 38 min). Comparison of geometric means of AUCo-tlast of the model drug confirmed this observation with 10 times higher value after fed administration. Urinary excretion of sodium well reflected the increased sodium-reuptake inhibition due to higher furosemide exposure under fed conditions. However, the poor performance after fasted intake of the system is in line with data from several other gastroretentive formulations. The present study highlighted the value of novel test methods during the development of gastroretentive formulations. Yet, a system with reproducible gastroretentive properties especially under fasted conditions has to be designed.
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