A dual pH- and reduction-responsive anticancer drug
delivery system based on PEG-SS-poly(amino acid) block copolymer
Li, BQ (Li, Bingqiang)[ 1 ] ; Shan, M (Shan, Meng)[ 1 ] ; Di, X (Di, Xiang)[ 1 ] ; Gong, C (Gong, Chu)[ 1 ] ; Zhang, LH (Zhang, Lihua)[ 2 ] ; Wang, YM (Wang, Yanming)[ 2 ] ; Wu, GL (Wu, Guolin)[ 1 ]
RSC ADVANCES,
2017, 7(48): 30242-30249
DOI: 10.1039/c7ra04254j
WOS:000403565400041
Abstract
A pH- and
reduction-responsive anticancer drug delivery system was prepared and the
triggerable and controllable drug release in response to stimuli was observed.
In the first step, methoxy-poly(ethylene glycol) (mPEG) was conjugated with
polysuccinimide (PSI) via disulfide linkages, and the PSI segment thereafter,
was aminolyzed by 2-diisopropylaminoethylamine (DIPEA) and hydrazine hydrate (Hy).
The obtained amphiphilic copolymer could form a bond with the model drug
doxorubicin (DOX) at pH 7.4 via acid-labile hydrazone bonds, and more free DOX
molecules could be encapsulated via hydrophobic interactions and p-p stacking
between the aromatic rings, leading to DOX-loaded micelles formation. These
polymers and polymeric micelles then were characterized. The results showed
that the polymeric micelles exhibited dual pH-and reduction-responsive
disassembly behaviors. Moreover, while the blank copolymers had excellent
cytocompatibility, the DOX-loaded micelles showed an enhanced drug release
profile and improved cytotoxicity with decrease of pH and/or the addition of
glutathione (GSH). These results indicated that the novel nanoparticle based on
PEG-SS-poly(amino acid) block copolymer is a promising candidate for a carrier
in controllable anti-tumor drug delivery.
