Self-stabilized, hydrophobic or PEGylated paclitaxel polymer prodrug nanoparticles for cancer therapy

被引:25
作者
Bao, Yinyin [1 ]
Guegain, Elise [1 ]
Mougin, Julie [1 ]
Nicolas, Julien [1 ]
机构
[1] Univ Paris Sud, CNRS, UMR 8612, Inst Galien Paris Sud,Fac Pharm, 5 Rue Jean Baptiste Clement, F-92290 Chatenay Malabry, France
关键词
NITROXIDE-MEDIATED POLYMERIZATION; RING-OPENING POLYMERIZATION; DRUG-DELIVERY; CREMOPHOR EL; PHASE-II; IN-VIVO; TAXOL; CONJUGATE; AGGREGATION; HYPERSENSITIVITY;
D O I
10.1039/c7py01918a
中图分类号
O63 [高分子化学(高聚物)];
学科分类号
070305 ; 080501 ; 081704 ;
摘要
Facile derivatization of paclitaxel (Ptx) and subsequent "drug-initiated" synthesis of well-defined Ptx-polymer prodrugs was performed from nitroxide-mediated polymerization or reversible addition-fragmentation chain transfer polymerization. Short polyisoprene (M-n = 2640-4310 g mol(-1), D similar to 1.1) or poly[(oligo(ethylene glycol) methyl ether methacrylate)] (M-n = 5580-7530 g mol(-1), D similar to 1.2) chains were grown from Ptx in a controlled fashion and enabled, for the first time, the formation of either self-stabilized, all-hydrophobic Ptx-polymer prodrug nanoparticles or their PEGylated counterparts. They exhibited average diameters in the 110-235 nm range, great colloidal stability in PBS and cell culture medium, high drug loadings (up to 32 wt%) and cytotoxicity similar to that of the parent drug on three different cancer cell lines (A549, L1210 and MCF-7). This versatile approach is expected to provide more potent anticancer nanocarriers and rejuvenate the development of Ptx-based nanomedicines.
引用
收藏
页码:687 / 698
页数:12
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