Organocatalytic Anticancer Drug Loading of Degradable Polymeric Mixed Micelles via a Biomimetic Mechanism
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- 作者:Julian M. W. Chan ; Jeremy P. K. Tan ; Amanda C. Engler ; Xiyu Ke ; Shujun Gao ; Chuan Yang ; Haritz Sardon ; Yi Yan Yang ; James L. Hedrick
- 刊名:Macromolecules
- 出版年:2016
- 出版时间:March 22, 2016
- 年:2016
- 卷:49
- 期:6
- 页码:2013-2021
- 全文大小:503K
- ISSN:1520-5835
文摘
Although self-assembled polymeric micelles have received significant attention as anticancer drug delivery systems, most of them suffer initial burst release of drugs after injection. Herein, a novel organocatalytic drug loading approach is reported to chemically conjugate anticancer drugs to the micellar core through an acid-labile bond that only breaks in the acidic tumor tissue and endolysosomal environments. Specifically, a degradable polymeric micelle system based on amphiphilic mPEG-b-polycarbonate block copolymers was developed. The mussel-inspired polymer design features catechol side chains to which the anticancer drug doxorubicin (DOX) can be covalently conjugated as pH-sensitive p-quinoneimines via a mechanism that mimics the Raper–Mason pathway of mammalian melanogenesis. We demonstrate that a higher drug loading is achieved when N-methylimidazole is cointroduced during self-assembly as an organocatalyst. The DOX-loaded mixed micelles formed from a catechol-functionalized polycarbonate/PEG block copolymer and a sister polymer with imidazole side chains are kinetically stable and display no signs of premature drug release, but possess comparable cytotoxicity in cancer cells to free DOX by a pH-triggered intracellular release. Moreover, we show that the nanoparticles accumulate in tumors through the enhanced permeability and retention (EPR) effect, and that the DOX-loaded mixed micelles suppress tumor growth more effectively than free DOX without causing toxicity in a mouse breast cancer model.