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采用热熔挤出法制备提高生物利用度的环孢素 A 无定形固体分散体:配方、理化性质评价及体内评价。

Amorphous solid dispersions of cyclosporine A with improved bioavailability prepared via hot melt extrusion: Formulation, physicochemical characterization, and in vivo evaluation.

机构信息

Institute of Biopharmaceutical Research, Liaocheng University, Hunan Road, Liaocheng, Shandong 252059, People's Republic of China.

Institute of Biopharmaceutical Research, Liaocheng University, Hunan Road, Liaocheng, Shandong 252059, People's Republic of China.

出版信息

Eur J Pharm Sci. 2022 Jan 1;168:106036. doi: 10.1016/j.ejps.2021.106036. Epub 2021 Oct 9.

Abstract

In this study, the amorphous solid dispersions of cyclosporine A (CsA-ASDs) were prepared by hot melt extrusion (HME) with PVP K12 as carrier to improve the oral bioavailability of CsA. The polymers were screened by solubilization and recrystallization inhibition experiments, then the CsA-ASDs were prepared with optimized technological parameters and characterized on thermodynamics and morphology. The results showed that CsA was dispersed among PVP K12 as amorphous form in CsA-ASDs, and the infrared spectrum testified that there was possible hydrogen bond interaction between CsA and PVP K12. The in vivo pharmacokinetics of CsA formulations in rats were analyzed via LC-MS. The AUC of CsA-ASD tablets increased by 7.3 times compared to CsA bulk powder and 3.1 times in contrast to CsA-PM tablets, respectively. The experiment proved that CsA-ASD tablets significantly improved the dissolution and absorption of the drug. This study had a reference value for the bioavailability improvement of oral CsA preparations.

摘要

在这项研究中,采用热熔挤出(HME)技术,以 PVP K12 为载体,制备环孢素 A 的无定形固体分散体(CsA-ASDs),以提高环孢素 A 的口服生物利用度。通过溶出度和重结晶抑制实验筛选出聚合物,然后用优化的工艺参数制备 CsA-ASDs,并对其热力学和形态进行了表征。结果表明,CsA 以无定形形式分散在 PVP K12 中,红外光谱表明 CsA 与 PVP K12 之间可能存在氢键相互作用。通过 LC-MS 分析大鼠体内 CsA 制剂的药代动力学。与 CsA 原料药相比,CsA-ASD 片剂的 AUC 增加了 7.3 倍,与 CsA-PM 片剂相比增加了 3.1 倍。实验证明 CsA-ASD 片剂显著提高了药物的溶解和吸收。本研究对提高口服 CsA 制剂的生物利用度具有参考价值。

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