Synthesis and Anti-Melanoma Activity of L-Cysteine-Coated Iron Oxide Nanoparticles Loaded with Doxorubicin

被引:14
|
作者
Toderascu, Luiza Izabela [1 ,2 ]
Sima, Livia Elena [3 ]
Orobeti, Stefana [1 ,3 ]
Florian, Paula Ecaterina [3 ]
Icriverzi, Madalina [3 ]
Maraloiu, Valentin-Adrian [4 ]
Comanescu, Cezar [4 ,5 ]
Iacob, Nicusor [4 ]
Kuncser, Victor [4 ]
Antohe, Iulia [1 ]
Popescu-Pelin, Gianina [1 ]
Stanciu, George [1 ]
Ionita, Petre [2 ]
Mihailescu, Cristian N. N. [1 ]
Socol, Gabriel [1 ]
机构
[1] Natl Inst Laser Plasma & Radiat Phys, Magurele 077125, Ilfov, Romania
[2] Univ Bucharest, Fac Chem, Bucharest 050663, Romania
[3] Romanian Acad, Inst Biochem, Bucharest 060031, Romania
[4] Natl Inst Mat Phys, Magurele 077125, Ilfov, Romania
[5] Univ Bucharest, Fac Phys, Magurele 077125, Ilfov, Romania
关键词
magnetic nanoparticles; melanoma; L-Cys; Dox; chemotherapeutic; FUNCTIONALIZED MAGNETIC NANOPARTICLES; RAY PHOTOELECTRON-SPECTROSCOPY; DRUG-DELIVERY SYSTEMS; NANOCARRIERS; MANAGEMENT; CARRIERS; OXYGEN; FE3O4; PH;
D O I
10.3390/nano13040621
中图分类号
O6 [化学];
学科分类号
0703 ;
摘要
In this study, we report on the synthesis of L-Cysteine (L-Cys)-coated magnetic iron oxide nanoparticles (NPs) loaded with doxorubicin (Dox). The Fe3O4-L-Cys-Dox NPs were extensively characterized for their compositional and morpho-structural features using EDS, SAED, XRD, FTIR and TEM. XPS, Mossbauer spectroscopy and SQUID measurements were also performed to determine the electronic and magnetic properties of the Fe3O4-L-Cys-Dox nanoparticles. Moreover, by means of a FO-SPR sensor, we evidenced and confirmed the binding of Dox to L-Cys. Biological tests on mouse (B16F10) and human (A375) metastatic melanoma cells evidenced the internalization of magnetic nanoparticles delivering Dox. Half maximum inhibitory concentration IC50 values of Fe3O4-L-Cys-Dox were determined for both cell lines: 4.26 mu g/mL for A375 and 2.74 mu g/mL for B16F10, as compared to 60.74 and 98.75 mu g/mL, respectively, for unloaded controls. Incubation of cells with Fe3O4-L-Cys-Dox modulated MAPK signaling pathway activity 3 h post-treatment and produced cell cycle arrest and increased apoptosis by 48 h. We show that within the first 2 h of incubation in physiological (pH = 7.4) media, similar to 10-15 mu M Dox/h was released from a 200 mu g/mL Fe3O4-L-Cys-Dox solution, as compared to double upon incubation in citrate solution (pH = 3), which resembles acidic environment conditions. Our results highlight the potential of Fe3O4-L-Cys-Dox NPs as efficient drug delivery vehicles in melanoma therapy.
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页数:23
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