Enhanced drug delivery to cancer cells through a pH-sensitive polycarbonate platform

被引:2
|
作者
Arno, Maria C. C. [1 ,2 ]
Simpson, Joshua D. D. [3 ,4 ,5 ]
Blackman, Lewis D. D. [6 ]
Brannigan, Ruairi P. [6 ]
Thurecht, Kristofer J. J. [3 ,4 ,5 ]
Dove, Andrew P. P. [1 ]
机构
[1] Univ Birmingham, Sch Chem, Birmingham B15 2TT, England
[2] Univ Birmingham, Inst Canc & Genom Sci, Birmingham B15 2TT, England
[3] Univ Queensland, Australian Inst Bioengn & Nanotechnol, St Lucia, Qld 4072, Australia
[4] Univ Queensland, Ctr Adv Imaging, St Lucia, Qld 4072, Australia
[5] Univ Queensland, ARC Ctr Excellence Convergent Bionano Sci & Techno, St Lucia, Qld 4072, Australia
[6] Univ Warwick, Dept Chem, Coventry CV4 7AL, England
基金
澳大利亚研究理事会; 英国工程与自然科学研究理事会; 英国医学研究理事会; 英国生物技术与生命科学研究理事会;
关键词
POLYMERIC MICELLES; BLOCK-COPOLYMERS; PHASE-I; RELEASE; NANOPARTICLES; ACETAL; CAMPTOTHECIN; NANOCARRIERS; ENDOCYTOSIS; DOXORUBICIN;
D O I
10.1039/d2bm01626e
中图分类号
TB3 [工程材料学]; R318.08 [生物材料学];
学科分类号
0805 ; 080501 ; 080502 ;
摘要
Polymer-drug conjugates are widely investigated to enhance the selectivity of therapeutic drugs to cancer cells, as well as increase circulation lifetime and solubility of poorly soluble drugs. In order to direct these structures selectively to cancer cells, targeting agents are often conjugated to the nanoparticle surface as a strategy to limit drug accumulation in non-cancerous cells and therefore reduce systemic toxicity. Here, we report a simple procedure to generate biodegradable polycarbonate graft copolymer nanoparticles that allows for highly efficient conjugation and intracellular release of S-(+)-camptothecin, a topoisomerase I inhibitor widely used in cancer therapy. The drug-polymer conjugate showed strong efficacy in inhibiting cell proliferation across a range of cancer cell lines over non-cancerous phenotypes, as a consequence of the increased intracellular accumulation and subsequent drug release specifically in cancer cells. The enhanced drug delivery towards cancer cells in vitro demonstrates the potential of this platform for selective treatments without the addition of targeting ligands.
引用
收藏
页码:908 / 915
页数:8
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