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Core–Shell–Corona Micelle Stabilized by Reversible Cross‐Linkage for Intracellular Drug Delivery
Author(s) -
Wang YuCai,
Li Yang,
Sun TianMeng,
Xiong MengHua,
Wu Juan,
Yang YiYan,
Wang Jun
Publication year - 2010
Publication title -
macromolecular rapid communications
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 1.348
H-Index - 154
eISSN - 1521-3927
pISSN - 1022-1336
DOI - 10.1002/marc.200900863
Subject(s) - micelle , ethylene glycol , copolymer , amphiphile , polymer chemistry , drug delivery , polymerization , chemistry , drug carrier , materials science , polymer , chemical engineering , organic chemistry , aqueous solution , engineering
Reversibly cross‐linked core–shell–corona micelles based on a triblock copolymer composed of poly(aliphatic ester), polyphosphoester, and poly(ethylene glycol) are reported. The triblock copolymer is synthesized through consecutive ring‐opening polymerization of ε‐ caprolactone and 2,4‐dinitrophenylthioethyl ethylene phosphate, followed by conjugation of poly(ethylene glycol). After deprotection under mild conditions, the amphiphilic polymer forms core–shell–corona micelles with free thiols in the shell. Cross‐linking of the micelles within the shell reduces their critical micellization concentration and enhances their stability against severe conditions. The redox‐sensitive cross‐linkage allows the facilitated release of entrapped anticancer drugs in the cytoplasm in response to the intracellular reductive environment. With enhanced stability during circulation after administration, and accelerated intracellular drug release at the target site, the biocompatible and biodegradable shell‐cross‐linked polymeric micelle is promising as a drug vehicle for cancer chemotherapy.