In vitro and in vivo anticancer effect of pH-responsive paclitaxel-loaded niosomes

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作者
Mahmood Barani
Mohammad Reza Hajinezhad
Saman Sargazi
Abbas Rahdar
Sheida Shahraki
Azadeh Lohrasbi-Nejad
Francesco Baino
机构
[1] Kerman University of Medical Sciences,Medical Mycology and Bacteriology Research Center
[2] University of Zabol,Basic Veterinary Science Department, Veterinary Faculty
[3] Research Institute of Cellular and Molecular Sciences in Infectious Diseases,Cellular and Molecular Research Center
[4] University of Zabol,Department of Physics
[5] Shahid Bahonar University of Kerman,Department of Agricultural Biotechnology
[6] Politecnico di Torino,Institute of Materials Physics and Engineering, Department of Applied Science and Technology
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摘要
In this study, paclitaxel (PTX)-loaded pH-responsive niosomes modified with ergosterol were developed. This new formulation was characterized in terms of size, morphology, encapsulation efficiency (EE), and in vitro release at pH 5.2 and 7.4. The in vitro efficacy of free PTX and niosome/PTX was assessed using MCF7, Hela, and HUVEC cell lines. In order to evaluate the in vivo efficacy of niosomal PTX in rats as compared to free PTX, the animals were intraperitoneally administered with 2.5 mg/kg and 5 mg/kg niosomal PTX for two weeks. Results showed that the pH-responsive niosomes had a nanometric size, spherical morphology, 77% EE, and pH-responsive release in pH 5.2 and 7.4. Compared with free PTX, we found markedly lower IC50s when cancer cells were treated for 48 h with niosomal PTX, which also showed high efficacy against human cancers derived from cervix and breast tumors. Moreover, niosomal PTX induced evident morphological changes in these cell lines. In vivo administration of free PTX at the dose of 2.5 mg/kg significantly increased serum biochemical parameters and liver lipid peroxidation in rats compared to the control rats. The situation was different when niosomal PTX was administered to the rats: the 5 mg/kg dosage of niosomal PTX significantly increased serum biochemical parameters, but the group treated with the 2.5 mg/kg dose of niosomal PTX showed fewer toxic effects than the group treated with free PTX at the same dosage. Overall, our results provide proof of concept for encapsulating PTX in niosomal formulation to enhance its therapeutic efficacy.
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