Anticancer Drug-Loaded Nanospheres Based on Biodegradable Amphiphilic ε-Caprolactone and Carbonate Copolymers

被引:35
作者
Yan, Guo-Ping [1 ]
Zong, Rong-Feng [1 ]
Li, Liang [1 ]
Fu, Ting [1 ]
Liu, Fan [1 ]
Yu, Xiang-Hua [1 ]
机构
[1] Wuhan Inst Technol, Sch Mat Sci & Engn, Wuhan 430074, Peoples R China
基金
中国国家自然科学基金;
关键词
biodegradable polycarbonate; copolymers; drug controlled release; nanospheres; sulfadiazine; RING-OPENING COPOLYMERIZATION; TRIMETHYLENE CARBONATE; POLYMERIZATION; ACID; POLYASPARTAMIDE; NANOPARTICLES; POLYMERS; DELIVERY;
D O I
10.1007/s11095-010-0275-7
中图分类号
O6 [化学];
学科分类号
0703 ;
摘要
The aim was to investigate anticancer drug-loaded poly(carbonate-ester) nanospheres as potential drug delivery systems for cancer therapy. Functional poly(carbonate-ester) copolymers (HPCP-SD) were synthesized by the incorporation of sulfadiazine as the tumor-targeting groups to hydroxyl groups of poly(carbonate-ester) copolymers. Two types of anticancer drug-loaded poly(carbonate-ester) nanospheres I and II were further prepared by dialysis method and high-voltage electrostatic field-assisted atomization, respectively, using HPCP-SD as polymeric carriers. These carriers and anticancer drug-loaded nanospheres were characterized, and their properties in vitro and in vivo were evaluated. These anticancer drug-loaded poly(carbonate-ester) nanospheres had steady drug release rates and good controlled release properties. Moreover, anticancer drug-loaded poly(carbonate-ester) nanospheres II had faster drug release rates than those of anticancer drug-loaded nanospheres I. These anticancer drug-loaded nanospheres possessed lower cytotoxicity to HEK 293 cells and exhibited obviously higher anticancer efficiencies to the HeLa tumor cells than that of 5-fluorouracil. Anticancer drug-loaded nanospheres I possessed lower cytotoxicity to HEK 293 cells and higher anticancer activity to HeLa cells than those of anticancer drug-loaded nanospheres II. These anticancer drug-loaded poly(carbonate-ester) nanospheres showed the potential as drug delivery systems for cancer therapy.
引用
收藏
页码:2743 / 2752
页数:10
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