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Characterization and evaluation of a self-microemulsifying drug delivery system containing tectorigenin,an isoflavone with low aqueous solubility and poor permeability
Authors:Yunrong Zhang  Li He  Shanlan Yue  Qingting Huang  Yuhong Zhang
Affiliation:1. West China School of Pharmacy, Sichuan University, Chengdu, China,;2. Chengdu Women and Children’s Central Hospital, Chengdu, China, and;3. Medical College of China Three Gorges University, Yichang, China
Abstract:The purpose of this study was to characterize and evaluate tectorigenin-loaded self-microemulsifying drug delivery system (TG-SMEDDS), a previously studied preparation, and further confirm the improvement of TG in solubility and bioavailability. The appearance of TG-SMEDDS was clear and transparent, with good mobility. The microemulsion formed by TG-SMEDDS was globular, edge smooth, clear-cut, and distribution homogeneous under transmission electron microscope. The stability studies revealed that TG-SMEDDS remained stable at room temperature for at least 3 months. TG-SMEDDS showed excellent dissolution behavior that more than 90% of TG was released in only 5?min. The in situ intestinal perfusion studies indicated enhancement of absorption in four tested intestinal segments, and the main absorption site of TG was changed to duodenum. In addition, TG-SMEDDS showed significantly higher Cmax and AUC values (11-fold and 5-fold higher values, respectively; P?AUC0-t of crude TG and TG-SMEDDS in bile duct non-ligation rats were 6.05 and 2.80 times, respectively, than that in bile duct ligation rats, indicating the existence of enterohepatic circulation and the secretion of bile could significantly affect the absorption of TG. Further studies showed that even the bile duct was ligation, TG-SMEDDS can still keep a better oral bioavailability (179.67%, compared with crude TG in the bile duct non-ligation rats). Therefore, our study implies that SMEDDS containing TG could be an effective strategy for the oral administration of TG.
Keywords:Tectorigenin  self-microemulsifying drug delivery system  in situ gastric and intestine perfusion  bioavailability  enterohepatic circulation
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