Investigation on Physicochemical Characteristics of a Nanoliposome-Based System for Dual Drug Delivery

被引:36
|
作者
Nam, Jae Hyun [1 ]
Kim, So-Yeon [1 ]
Seong, Hasoo [1 ]
机构
[1] Korea Res Inst Chem Technol, Therapeut & Biotechnol Div, 141 Gajeong Ro, Deajeon 34114, South Korea
来源
关键词
Nanoliposome; Dual drug delivery system; Ultrasonication; Remote loading technology; Time-differential release; BREAST-CANCER; LIPOSOMES; DOXORUBICIN; ERLOTINIB; DRIVEN; ENCAPSULATION; COMBINATION; ACTIVATION; STABILITY; VESICLES;
D O I
10.1186/s11671-018-2519-0
中图分类号
TB3 [工程材料学];
学科分类号
0805 ; 080502 ;
摘要
Synergistic effects of multiple drugs with different modes of action are utilized for combinatorial chemotherapy of intractable cancers. Translation of in vitro synergistic effects into the clinic can be realized using an efficient delivery system of the drugs. Despite a few studies on nano-sized liposomes containing erlotinib (ERL) and doxorubicin (DOX) in a single liposome vesicle, reliable and reproducible preparation methods as well as physicochemical characteristics of a non-PEGylated nanoliposome co-encapsulated with ERL and DOX have not been yet elucidated. In this study, ERL-encapsulated nanoliposomes were prepared using the lipid film-hydration method. By ultrasonication using a probe sonicator, the liposome diameter was reduced to less than 200 nm. DOX was loaded into the ERL-encapsulated nanoliposomes using ammonium sulfate (AS)-gradient or pH-gradient method. Effects of DOX-loading conditions on encapsulation efficiency (EE) of the DOX were investigated to determine an efficient drug-loading method. In the EE of DOX, AS-gradient method was more effective than pH gradient. The dual drug-encapsulated nanoliposomes had more than 90% EE of DOX and 30% EE of ERL, respectively. Transmission electron microscopy and selected area electron diffraction analyses of the dual drug-encapsulated nanoliposomes verified the highly oriented DOX-sulfate crystals inside the liposome as well as the less oriented small crystals of ERL in the outermost region of the nanoliposome. The nanoliposomes were stable at different temperatures without an increase of the nanoliposome diameter. The dual drug-encapsulated nanoliposomes showed a time-differential release of ERL and DOX, implying proper sequential releases for their synergism. The preparation methods and the physicochemical characteristics of the dual drug delivery system contribute to the development of the optimal process and more advanced systems for translational researches.
引用
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页数:11
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