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口服异乐定前体脂质体的处方前研究、评价及药代动力学。

Formulation, evaluation, and pharmacokinetics of isradipine proliposomes for oral delivery.

机构信息

Department of Industrial Pharmacy, St. Peter's Institute of Pharmaceutical Sciences, Warangal, India.

出版信息

J Liposome Res. 2012 Dec;22(4):285-94. doi: 10.3109/08982104.2012.697067. Epub 2012 Jul 4.

Abstract

Proliposomes loaded with isradipine were prepared successfully to enhance the oral bioavailability of isradipine. In this study, proliposomes were prepared by film deposition by the carrier method with varying ratios of hydrogenated soy phosphatidyl choline (HSPC) and cholesterol using spray-dried mannitol (Pearlitol SD 200) as the carrier. The formulation containing an equimolar ratio of HSPC and cholesterol showed smaller vesicle size, high surface charge, and entrapment efficiency. The formation of liposomes and surface morphology of optimized proliposome formulation was studied by optical and scanning electron microscopy, respectively. Fourier transform infrared, differential scanning calorimetry, and powder X-ray diffractometry studies were performed to assess the solid-state characteristics of the formulation. Ex vivo permeation enhancement assessed from flux, permeability coefficient, and enhancement ratio were significantly higher for proliposomes, compared to control. The pharmacokinetic parameters were evaluated in male albino Wistar rats, and a significant improvement in bioavailability (2.4-fold) was observed from the optimized proliposome formulation, compared to control (oral suspension). The stability study revealed that the formulations are stable when stored at 4°C.

摘要

成功制备了包载异搏定的前体脂质体,以提高异搏定的口服生物利用度。在这项研究中,采用载体法,以氢化大豆磷脂酰胆碱(HSPC)和胆固醇的不同比例,通过薄膜沉积法制备前体脂质体,以喷雾干燥甘露醇(Pearlitol SD 200)为载体。含有 HSPC 和胆固醇等摩尔比的配方具有较小的囊泡粒径、高表面电荷和包封效率。采用光学显微镜和扫描电子显微镜分别研究了脂质体的形成和优化前体脂质体配方的表面形态。傅里叶变换红外、差示扫描量热法和粉末 X 射线衍射法研究用于评估配方的固态特性。与对照品相比,前体脂质体的体外渗透增强评估显示通量、渗透系数和增强比均显著提高。在雄性白化 Wistar 大鼠中评价了药代动力学参数,与对照品(口服混悬液)相比,从优化的前体脂质体制剂中观察到生物利用度显著提高(2.4 倍)。稳定性研究表明,制剂在 4°C 下储存时稳定。

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