Amphiphilic Glycopolypeptide Star Copolymer-Based Cross-Linked Nanocarriers for Targeted and Dual-Stimuli-Responsive Drug Delivery

被引:43
|
作者
Pandey, Bhawana [1 ,3 ]
Patil, Naganath G. [1 ,3 ]
Bhosle, Govind S. [2 ,3 ]
Arnbade, Ashootosh V. [1 ,3 ]
Sen Gupta, Sayam [4 ]
机构
[1] CSIR Natl Chem Lab, Polymer Sci & Engn Div, Dr Homi Bhabha Rd, Pune 411008, Maharashtra, India
[2] CSIR Natl Chem Lab, Organ Chem Div, Dr Homi Bhabha Rd, Pune 411008, Maharashtra, India
[3] Acad Sci & Innovat Res AcSIR, New Delhi 110025, India
[4] Indian Inst Sci Educ & Res, Dept Chem Sci, Kolkata 741246, India
关键词
INTRACELLULAR DRUG; MICELLES; NANOPARTICLES; REDUCTION; VESICLES; PH; POLYMERS; RELEASE; POLYMERIZATION; DOXORUBICIN;
D O I
10.1021/acs.bioconjchem.8b00831
中图分类号
Q5 [生物化学];
学科分类号
071010 ; 081704 ;
摘要
Glycopolypeptide-based nanocarriers are an attractive class of drug delivery vehicles because of the involvement of carbohydrates in the receptor-mediated endocytosis process. To enhance their efficacy toward controlled and programmable drug delivery, we have prepared stable glycopolypeptide-based bioactive dual-stimuli-responsive (redox and enzyme) micelles for delivery of anticancer drugs specifically to the cancer cells. The amphiphilic biocompatible miktoarm star copolymer, which comprises two hydrophobic poly(epsilon-caprolactone) blocks, a short poly-(propargyl glycine) middle block, and a hydrophilic galactose glycopolypeptide block, was designed and synthesized. The star copolymer is initially self-assembled into un-cross-linked (UCL) micelles, and free alkyne groups at the core shell interface of the UCL micelles, which were cross-linked by bis(azidoethyl) disulfide (BADS) via click chemistry to form interface cross linked (ICL) micelles. ICL micelles were found to be stable against dilution. BADS imparted redox-responsive properties to the micelles, while PCL rendered them enzyme-degradable. Dual-stimuli-responsive release behavior with Dox as model drug was studied individually as well as synergistically by applying two stimuli in different sequences. The galactose-containing UCL and ICL micelles were shown to be nontoxic. Intracellular Dox release from UCL and ICL micelles was demonstrated in liver cancer cells (HepG2) by time-dependent cellular uptake studies, and controlled release from ICL micelles compared to UCL micelles was observed. The present report opens a new approach toward targeted and programmable drug delivery in tumor tissues via a specifically targeted (receptor-mediated), dual-responsive, and stable cross-linked nanocarrier system.
引用
收藏
页码:633 / 646
页数:14
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