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β-环糊精诱导的单层反离子囊泡的稳定化:一种可调节的药物输送库的策略。

Stabilization of unilamellar catanionic vesicles induced by β-cyclodextrins: A strategy for a tunable drug delivery depot.

机构信息

Department of Chemical and Pharmaceutical Sciences, University of Trieste, via L. Giorgieri 1, 34127 Trieste, Italy.

Coimbra Chemistry Centre, Dept. of Chemistry, University of Coimbra, Rua Larga, Coimbra, Portugal.

出版信息

Int J Pharm. 2018 Sep 5;548(1):474-479. doi: 10.1016/j.ijpharm.2018.07.026. Epub 2018 Jul 7.

Abstract

The limited stability of catanionic vesicles has discouraged their wide use for encapsulation and controlled release of active substances. Their structure can easily break down to form lamellar phases, micelles or rearrange into multilamellar vesicles, as a consequence of small changes in their composition. However, despite the limited stability, catanionic vesicles possess an attractive architecture, which is able to efficiently encapsulate both hydrophobic and hydrophilic molecules. Therefore, improving the stability of the vesicles, as well as the control on unilamellar structures, are prerequisites for their wider application range. This study focuses on the impact of β-cyclodextrins for the stabilization of SDS/CTAB catanionic vesicles. Molar ratio and sample preparation procedures have been investigated to evaluate the temperature stability of catanionic vesicles. Diffusion and spectroscopic techniques evidenced that when β-cyclodextrins are added, unilamellar structures are stabilized above the multilamellar-unilamellar vesicles critical temperature. The results evidence encouraging perspectives for the use of vesicular nanoreservoirs for drug depot applications.

摘要

双离子囊泡的稳定性有限,这阻碍了它们在活性物质包封和控制释放方面的广泛应用。由于其组成的微小变化,它们的结构很容易分解形成层状相、胶束或重新排列成多层囊泡。然而,尽管双离子囊泡的稳定性有限,但它们具有吸引人的结构,能够有效地包封疏水性和亲水性分子。因此,提高囊泡的稳定性以及对单层结构的控制是扩大其应用范围的前提条件。本研究重点研究了β-环糊精对 SDS/CTAB 双离子囊泡的稳定作用。研究了摩尔比和样品制备程序,以评估双离子囊泡的温度稳定性。扩散和光谱技术表明,当添加β-环糊精时,单层结构在多层-单层囊泡的临界温度以上得到稳定。这些结果为使用囊泡纳米储库进行药物库应用提供了令人鼓舞的前景。

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