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Preparation and pharmacokinetics in beagle dogs of ganershu sustained-release pellets

机译:甘尔舒缓释微丸在比格犬体内的制备及药代动力学

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Background:The active ingredients of Ganershu compound recipe, which are effective for hepatitis treatment in liver protection and transaminase reduction. However, the active ingredients of Ganershu compound recipe are poor absorption, which conduct it has a low oral bioavailability.Objective:We prepared Ganershu sustained-release pellets (GSPs) by fluidized-bed on central composite design-response surface methodology and increase its bioavailability in beagle dogs.Materials and Methods:In this study, GSPs were successfully prepared. The Drug-loaded pellets and sustained-release coated were carried out in fluidized-bed machine. GSP was optimized for fitting release, roundness, and the overall desirability by central composite design-response surface methodology.Results:To optimize cumulative release profile, the outermost ethyl cellulose coating layer and the hydroxypropyl methyl cellulose (HPMC) swelling layer were employed, which were respectively given coating levels in terms of weight gain of 22% and 6%, the concentration of HPMC is 4.5% (g/ml). The pharmacokinetics of Ganershu normal pellets (GNPs) and GSP was studied in beagle dogs after oral administration. The naringenin as an index, the area under the curve0-∞ of naringenin in GSP was 1.38 times greater than that of GNP. Meanwhile, Tmax of GSP was prolonged for about 74%.Conclusion:This study can clearly indicate that we enhanced the oral bioavailability of Ganershu by preparing the GSP, which had the sustained dissolution and improved the potential of it for clinical application.
机译:背景:肝二俞复方的有效成分,对肝炎的保护和转氨酶的减少有效。目的:通过流化床方法,在中央复合设计-响应面法上制备甘二舒缓释微丸,提高其生物利用度,但其有效成分吸收较差,口服生物利用度较低。材料与方法:在本研究中,成功​​制备了GSP。载药小丸和缓释包衣在流化床机中进行。结果:为了优化累积释放曲线,使用了最外层的乙基纤维素涂层和羟丙基甲基纤维素(HPMC)溶胀层,从而优化了GSP的贴合性,圆度和整体合意性。分别以22%和6%的增重给出涂料水平,HPMC的浓度为4.5%(g / ml)。口服后,在比格犬中研究了Ganershu正常小丸(GNPs)和GSP的药代动力学。以柚皮素为指标,GSP中柚皮素的曲线0-∞以下面积是GNP的1.38倍。同时,GSP的Tmax延长了约74%。

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