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Delivery of siRNA into breast cancer cells via phage fusion protein-targeted liposomes
被引:67
作者:
Bedi, Deepa
[1
]
Musacchio, Tiziana
[2
]
Fagbohun, Olusegun A.
[1
]
Gillespie, James W.
[1
]
Deinnocentes, Patricia
[1
]
Bird, R. Curtis
[1
]
Bookbinder, Lonnie
[3
]
Torchilin, Vladimir P.
[2
]
Petrenko, Valery A.
[1
]
机构:
[1] Auburn Univ, Coll Vet Med, Dept Pathobiol, Auburn, AL 36849 USA
[2] Northeastern Univ, Dept Pharmaceut Sci, Boston, MA 02115 USA
[3] Calvert Res Inst LLC, Cary, NC USA
关键词:
siRNA;
Liposomes;
Major coat protein;
Phage display;
Targeted delivery;
Breast cancer;
COAT PROTEIN;
THERAPEUTIC-EFFICACY;
ENHANCED BINDING;
DRUG-DELIVERY;
GENE DELIVERY;
TUMOR-CELLS;
LIBRARIES;
PEPTIDES;
DISPLAY;
LIGANDS;
D O I:
10.1016/j.nano.2010.10.004
中图分类号:
TB3 [工程材料学];
学科分类号:
0805 ;
080502 ;
摘要:
Efficacy of siRNAs as potential anticancer therapeutics can be increased by their targeted delivery into cancer cells via tumor-specific ligands. Phage display offers a unique approach to identify highly specific and selective ligands that can deliver nanocarriers to the site of disease. In this study, we proved a novel approach for intracellular delivery of siRNAs into breast cancer cells through their encapsulation into liposomes targeted to the tumor cells with preselected intact phage proteins. The targeted siRNA liposomes were obtained by a fusion of two parental liposomes containing spontaneously inserted siRNA and fusion phage proteins. The presence of pVIII coat protein fused to a MCF-7 cell-targeting peptide DMPGTVLP in the liposomes was confirmed by Western blotting. The novel phage-targeted siRNA-nanopharmaceuticals demonstrate significant down-regulation of PRDM14 gene expression and PRDM14 protein synthesis in the target MCF-7 cells. This approach offers the potential for development of new anticancer siRNA-based targeted nanomedicines. From the Clinical Editor: In this study, the authors report a novel approach for targeted intracellular delivery of siRNAs into breast cancer cells through encapsulation into liposomes targeted to the tumor cells with preselected intact phage proteins. (C) 2011 Elsevier Inc. All rights reserved.
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页码:315 / 323
页数:9
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