Preparation, characterization, and in vitro evaluation of bleomycin-containing nanoliposomes

被引:14
作者
Chiani, Mohsen [1 ]
Shokrgozar, Mohammad Ali [2 ]
Azadmanesh, Kayhan [3 ]
Norouzian, Dariush [1 ]
Mehrabi, Mohammad Reza [1 ]
Najmafshar, Aazam [4 ]
Akbarzadeh, Azim [1 ]
机构
[1] Inst Pasteur, Pilot Nanobiotechnol Dept, Tehran, Iran
[2] Inst Pasteur, Nat Cell Bank, Tehran, Iran
[3] Inst Pasteur, Dept Virol, Tehran, Iran
[4] Isfahan Univ Med Sci, Fac Pharm, Dept Clin Biochem, Esfahan, Iran
关键词
bleomycin; cytotoxicity; drug delivery; nanoliposomes; LIPOSOMES; RELEASE; NANOPARTICLES; ENCAPSULATION; NANOCARRIERS; CELLS;
D O I
10.1111/cbdd.12869
中图分类号
Q5 [生物化学]; Q7 [分子生物学];
学科分类号
071010 ; 081704 ;
摘要
Bleomycin is an anticancer drug used against various types of cancers. The aim of this study was to prepare a new PEGylated and non-PEGylated nanoliposomal formulation of bleomycin (PEG-nLip-BLM and nLip-BLM) and evaluate their anticancer activity in different tumor cell lines. The liposomes were prepared by thin-film hydration method, and then, bleomycin (BLM) was loaded to the prepared vesicles. The size, zeta potential, entrapment efficiency, loading rate, release profile, and cytotoxicity of liposomal formulations in TC-1, LLC1, and HFLF-PI5 cell lines were investigated. Mean particle size and zeta potential of the PEG-nLip-BLM and nLip- BLM were found to be 99.4 +/- 4.6 nm and -34.83 +/- 4.7 mV; and 112.2 +/- 7.2 nm and -27.5 +/- 3.2 mV, respectively, which were stable for at least 2 months. Encapsulation and loading efficiency of BLM for PEG-nLip-BLM and nLip-BLM were obtained about 83.1 +/- 4.2% and 14.3 +/- 2.5%; and 78.3 +/- 8.6% and 11.1 +/- 3.3%, respectively. Drug release study showed a slow release pattern without considerable burst effect. The liposomal formulations indicated lower toxicity compared to free drug in case of TC-1 and HFLF-PI5 cells, but their cytotoxicity against LLC1 cells was significantly higher than free drug. The results of this study indicated that PEG-nLip-BLM can be a suitable candidate for drug delivery to solid tumors.
引用
收藏
页码:492 / 497
页数:6
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