Efficient nonviral transfection of dendritic cells and their use for in vivo immunization

被引:0
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作者
Alistair S. Irvine
Peter K.E. Trinder
David L. Laughton
Helen Ketteringham
Ruth H. McDermott
Sophie C.H. Reid
Adrian M.R. Haines
Abdu Amir
Rhonda Husain
Rajeev Doshi
Lawrence S. Young
Andrew Mountain
机构
[1] Cobra Therapeutics,Lead Generation Biology
[2] The Science Park,undefined
[3] University of Keele,undefined
[4] CRC Institute of Cancer Studies,undefined
[5] University of Birmingham,undefined
[6] AstraZeneca R&D Charnwood,undefined
[7] Manchester Innovation Ltd.,undefined
来源
Nature Biotechnology | 2000年 / 18卷
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摘要
Immunization with dendritic cells (DCs) transfected with genes encoding tumor-associated antigens (TAAs) is a highly promising approach to cancer immunotherapy. We have developed a system, using complexes of plasmid DNA expression constructs with the cationic peptide CL22, that transfects human monocyte-derived DCs much more efficiently than alternative nonviral agents. After CL22 transfection, DCs expressing antigens stimulated autologous T cells in vitro and elicited primary immune responses in syngeneic mice, in an antigen-specific manner. Injection of CL22-transfected DCs expressing a TAA, but not DCs pulsed with a TAA-derived peptide, protected mice from lethal challenge with tumor cells in an aggressive model of melanoma. The CL22 system is a fast and efficient alternative to viral vectors for engineering DCs for use in immunotherapy and research.
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页码:1273 / 1278
页数:5
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