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Enhancement of Cytotoxicity and Inhibition of Angiogenesis in Oral Cancer Stem Cells by a Hybrid Nanoparticle of Bioactive Quinacrine and Silver: Implication of Base Excision Repair Cascade
被引:54
作者:
Satapathy, Shakti Ranjan
[1
]
Siddharth, Sumit
[1
]
Das, Dipon
[1
]
Nayak, Anmada
[1
]
Kundu, Chanakya Nath
[1
]
机构:
[1] KIIT Univ, KIIT Sch Biotechnol, Div Canc Biol, Bhubaneswar 751024, Orissa, India
关键词:
quinacrine;
silver;
hybrid nanoparticle;
oral cancer;
oral cancer stem cells;
OVERCOME MULTIDRUG-RESISTANCE;
BREAST EPITHELIAL-CELLS;
DRUG-RESISTANCE;
PARP INHIBITOR;
ANTICANCER ACTIVITY;
CO-DELIVERY;
CARCINOMA;
THERAPY;
DOXORUBICIN;
PATHWAY;
D O I:
10.1021/acs.molpharmaceut.5b00461
中图分类号:
R-3 [医学研究方法];
R3 [基础医学];
学科分类号:
1001 ;
摘要:
A poly(lactic-co-glycolic acid) (PLGA)-based uniform (50-100 nm) hybrid nanoparticle (QAgNP) with positive zeta potential (0.52 0.09 mV) was prepared by single emulsion solvent evaporation method with bioactive small molecule quinacrine (QC) in organic phase and silver (Ag) in aqueous phase. Physiochemical properties established it as a true hybrid nanoparticle and not a mixture of QC and Ag. Antitumor activity of QAgNP was evaluated by using various cancer cell lines including H-357 oral cancer cells and OSCC-cancer stem cell in an in vitro model system. QAgNP caused more cytotoxicity in cancer cells than normal epithelial cells by increasing BAX/BCL-XL, cleaved product PARP-1, and arresting the cells at S phase along with DNA damage. In addition, QAgNPs offered greater ability to kill the OSCC-CSCs compared to NQC and AgNPs. QAgNP offered anticancer action in OSCC-CSCs by inhibiting the base excision repair (BER) within the cells. Interestingly, alteration of BER components (Fen-1 and DNA polymerases (beta, delta, and epsilon) and unalteration of NHEJ (DNA-PKC) or HR (Rad-51) components was noted in QAgNP treated OSCC-CSC cells. Furthermore, QAgNP significantly reduced angiogenesis in comparison to physical mixture of NQC and AgNP in fertilized eggs. Thus, these hybrid nanoparticles caused apoptosis in OSCC-CSCs by inhibiting the angiogenesis and BER in cells.
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页码:4011 / 4025
页数:15
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