Functionalized diterpene parvifloron D-loaded hybrid nanoparticles for targeted delivery in melanoma therapy

被引:18
作者
Oliveira Silva, Catarina [1 ,2 ]
Molpeceres, Jesus [2 ]
Batanero, Belen [3 ]
Fernandes, Ana Sofia [1 ,4 ]
Saraiva, Nuno [1 ]
Costa, Joao Guilherme [1 ,4 ]
Rijo, Patricia [1 ,4 ]
Figueiredo, Isabel Vitoria [5 ,6 ]
Faisca, Pedro [7 ]
Reis, Catarina Pinto [1 ,8 ]
机构
[1] Univ Lusofona, Res Ctr Biosci & Hlth Technol, CBiOS, Campo Grande 376, P-1749024 Lisbon, Portugal
[2] Univ Alcala, Fac Pharm, Dept Biomed Sci, Alcala De Henares, Spain
[3] Univ Alcala, Fac Pharm, Dept Organ & Inorgan Chem, Alcala De Henares, Spain
[4] Univ Lisbon, Fac Pharm, Res Inst Med iMed ULisboa, Lisbon, Portugal
[5] Univ Coimbra, Fac Pharm, Pharmacol & Pharmaceut Care, Coimbra, Portugal
[6] Univ Coimbra, Inst Biomed Imaging & Life Sci, IBILI, Coimbra, Portugal
[7] Univ Lusofona, Fac Vet Med, Lisbon, Portugal
[8] Univ Lisbon, Fac Sci, Biophys & Biomed Engn, IBEB, Lisbon, Portugal
关键词
alpha-melanocyte-stimulating hormone; cutaneous melanoma; hybrid nanoparticles; parvifloron D; sustained release; targeted delivery;
D O I
10.4155/tde-2016-0027
中图分类号
R9 [药学];
学科分类号
1007 ;
摘要
Aim: Parvifloron D is a natural diterpene with a broad and not selective cytotoxicity toward human tumor cells. In order to develop a targeted antimelanoma drug delivery platform for Parvifloron D, hybrid nanoparticles were prepared with biopolymers and functionalized with alpha-melanocyte stimulating hormone. Results/methodology: Nanoparticles were produced according to a solvent displacement method and the physicochemical properties were assessed. It was shown that Parvifloron D is cytotoxic and can induce, both as free and as encapsulated drug, cell death in melanoma cells (human A375 and mouse B16V5). Parvifloron D-loaded nanoparticles showed a high encapsulation efficiency (87%) and a sustained release profile. In vitro experiments showed the nanoparticles' uptake and cell internalization. Conclusion: Hybrid nanoparticles appear to be a promising platform for long-term drug release, presenting the desired structure and a robust performance for targeted anticancer therapy.
引用
收藏
页码:521 / 544
页数:24
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