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基于β-乳球蛋白的无定形固体分散体:最新技术的图文综述。

β-Lactoglobulin-based amorphous solid dispersions: A graphical review on the state-of-the-art.

作者信息

Zhuo Xuezhi, Jasiukenaite Ieva, Löbmann Korbinian

机构信息

Zerion Pharma A/S, Fruebjergvej 3, 2100 Copenhagen, Denmark.

Zerion Pharma A/S, Fruebjergvej 3, 2100 Copenhagen, Denmark.

出版信息

Eur J Pharm Biopharm. 2024 Sep;202:114396. doi: 10.1016/j.ejpb.2024.114396. Epub 2024 Jul 4.

Abstract

Proteins have recently caught attention as potential excipients for amorphous solid dispersions (ASDs) to improve oral bioavailability of poorly water-soluble drugs. Notably, the studies have highlighted whey protein isolates, particularly β-lactoglobulin (BLG), as promising candidates in amorphous stabilization, dissolution and solubility enhancement, achieving drug loadings of 50 wt% and higher. Consequently, investigations into the mechanisms underlying the solid-state stabilization of amorphous drugs and the enhancement of drug solubility in solution have been conducted. This graphical review provides a comprehensive overview of recent findings concerning BLG-based ASDs. Firstly, the dissolution performance of BLG-based ASDs is compared to more traditional polymer-based ASDs. Secondly, the drug loading onto BLG and the resulting amorphous stabilization mechanisms is summarized. Thirdly, interactions between BLG and drug molecules in solution are described as the mechanisms governing the improvement of drug solubility. Lastly, we outline the impact of the spray drying process on the secondary structure of BLG, and the resulting differences in amorphous stabilization and drug dissolution performance between α-helix-rich and β-sheet-rich BLG-based ASDs.

摘要

蛋白质最近作为无定形固体分散体(ASD)的潜在辅料受到关注,以提高难溶性药物的口服生物利用度。值得注意的是,研究强调了乳清分离蛋白,特别是β-乳球蛋白(BLG),作为无定形稳定化、溶解和溶解度增强方面有前景的候选物,可实现50 wt%及更高的药物载量。因此,人们对无定形药物固态稳定化以及药物在溶液中溶解度增强的潜在机制进行了研究。本图文综述全面概述了关于基于BLG的ASD的最新研究成果。首先,将基于BLG的ASD的溶解性能与更传统的基于聚合物的ASD进行比较;其次,总结了药物在BLG上的载量以及由此产生的无定形稳定化机制;第三,描述了溶液中BLG与药物分子之间的相互作用,作为药物溶解度提高的潜在机制;最后,我们概述了喷雾干燥过程对BLG二级结构的影响,以及富含α-螺旋和富含β-折叠的基于BLG的ASD在无定形稳定化和药物溶解性能方面的差异。

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