Novel polymer micelle mediated co-delivery of doxorubicin and P-glycoprotein siRNA for reversal of multidrug resistance and synergistic tumor therapy

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作者
Chun-ge Zhang
Wen-jing Zhu
Yang Liu
Zhi-qiang Yuan
Shu-di Yang
Wei-liang Chen
Ji-zhao Li
Xiao-feng Zhou
Chun Liu
Xue-nong Zhang
机构
[1] College of Pharmaceutical Sciences,Department of Pharmaceutics
[2] Soochow University,undefined
[3] The first affiliated hospital of Soochow university,undefined
[4] College of Radiological Medicine and Protection,undefined
[5] Soochow University,undefined
[6] Changshu Hospital of Traditional Chinese Medicine,undefined
[7] The hospital of Suzhou People’s Hospital affiliated to Nanjing Medical University,undefined
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Co-delivery of chemotherapeutics and siRNA with different mechanisms in a single system is a promising strategy for effective cancer therapy with synergistic effects. In this study, a triblock copolymer micelle was prepared based on the polymer of N-succinyl chitosan–poly-L-lysine–palmitic acid (NSC–PLL–PA) to co-deliver doxorubicin (Dox) and siRNA–P-glycoprotein (P-gp) (Dox–siRNA-micelle). Dox–siRNA-micelle was unstable in pH 5.3 medium than in pH 7.4 medium, which corresponded with the in vitro rapid release of Dox and siRNA in acidic environments. The antitumor efficacy of Dox–siRNA-micelle in vitro significantly increased, especially in HepG2/ADM cells, which was due to the downregulation of P-gp. Moreover, almost all the Dox–siRNA-micelles accumulated in the tumor region beyond 24 h post-injection and the co-delivery system significantly inhibited tumor growth with synergistic effects in vivo. This study demonstrated the effectiveness of Dox–siRNA-micelles in tumor-targeting and MDR reversal and provided a promising strategy to develop a co-delivery system with synergistic effects for combined cancer therapy.
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