Focused ultrasound mediated drug delivery from temperature-sensitive liposomes: in-vitro characterization and validation

被引:22
作者
Escoffre, J-M [1 ]
Novell, A. [1 ]
de Smet, M. [2 ]
Bouakaz, A. [1 ]
机构
[1] PRES Ctr Val de Loire Univ, Univ Tours, UMR Inserm U930, Tours, France
[2] Biomed NMR, Dept Biomed Engn, Eindhoven, Netherlands
关键词
THERMOSENSITIVE LIPOSOMES; DOXORUBICIN DELIVERY; MILD HYPERTHERMIA; EFFICACY; RELEASE; CELL; NANOMEDICINE; FORMULATION; ABLATION; DOXIL(R);
D O I
10.1088/0031-9155/58/22/8135
中图分类号
R318 [生物医学工程];
学科分类号
0831 ;
摘要
Nanomedicine-based delivery with non-invasive techniques is a promising approach to increase local drug concentration and to reduce systemic side effects. Focused ultrasound (FUS) has become a promising strategy for non-invasive local drug delivery by mild hyperthermia. In this study, traditional temperature-sensitive liposomes (TTSLs) encapsulating doxorubicin (DOX) were evaluated for FUS-mediated drug delivery with an in-vitro FUS setup. In-vitro studies showed quantitative release of the DOX from the lumen of the temperature-sensitive liposomes when heated to 42 degrees C with FUS using 1 MHz sinusoidal waves at 1.75 MPa for 10 min. No release was observed when heated at 37 degrees C. Moreover, we showed that DOX released from TTSLs by FUS is as efficiently internalized by glioblastoma cells as free DOX at 37 degrees C. In-vitro therapeutic evaluation showed that exposure of a cell monolayer to FUS-activated TTSLs induced a 60% and a 50% decrease in cell viability compared to cell medium and to TTSLs preheated at 37 degrees C, respectively. Using an in-vitro 3D cell culture model, the results showed that after FUS-mediated hyperthermia, preheated liposomes induced a 1.7-fold decrease in U-87 MG spheroid growth in comparison to the preheated liposomes at 37 degrees C. In conclusion, our results show that in-vitro FUS allows the evaluation of TTSLs and does not modify the cellular uptake of the released DOX nor its cytotoxic activity.
引用
收藏
页码:8135 / 8151
页数:17
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