한빛사 논문
KAIST
Hyukjin Leea, Cheol‐Hee Ahnb, Tae Gwan Parka,*
aDepartment of Biological Sciences, Korea Advanced Institute of Science and Technology, Daejeon 305-701, South Korea
bDepartment of Materials Science and Engineering, Seoul National University, Seoul 151-744, South Korea
*To whom correspondence should be addressed.
Abstract
PLGA‐grafted HA copolymers were synthesized and utilized as target specific micelle carriers for DOX. For grafting hydrophobic PLGA chains onto the backbone of hydrophilic HA, HA was solubilized in an anhydrous DMSO by nano‐complexing with dimethoxy‐PEG. The carboxylic groups of HA were chemically grafted with PLGA, producing HA‐g‐PLGA copolymers. Resultant HA‐g‐PLGA self‐assembled in aqueous solution to form multi‐cored micellar aggregates and DOX was encapsulated during the self‐assembly. DOX‐loaded HA‐g‐PLGA micelle nanoparticles exhibited higher cellular uptake and greater cytotoxicity than free DOX for HCT‐116 cells that over‐expressed HA receptor, suggesting that they were taken up by the cells via HA receptor‐mediated endocytosis.
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