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Costimulation provided by DNA immunization enhances antitumor immunity.

M Corr, H Tighe, D Lee, J Dudler, M Trieu, D C Brinson and D A Carson
J Immunol November 15, 1997, 159 (10) 4999-5004;
M Corr
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H Tighe
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D Lee
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J Dudler
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M Trieu
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D C Brinson
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D A Carson
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Abstract

The interaction of the TCR with MHC class I-bound Ag is insufficient for the priming of CTL unless secondary costimulatory signals are provided. To ascertain the minimum elements required to activate an Ag-specific CTL response in vivo, we injected mice intradermally or i.m. with plasmid DNA encoding a MHC class I-restricted peptide Ag (minigene) and different membrane-bound costimulatory ligands. The minigene-encoded epitope only primed a specific CTL response if injected in the vicinity of an ectopically expressed costimulatory ligand. Vector encoding B7-1 was repeatedly more potent at stimulating a cytolytic response than vector encoding B7-2. In contrast the B7-2-encoding plasmid preferentially enhanced Ag-specific Ab responses when injected with either protein or a cDNA expression vector. Gene vaccination with plasmids encoding OVA and B7-1, but not B7-2, prolonged survival in mice challenged with an OVA-transfected tumor. These results show that functional B7-1 transfection can be achieved in vivo and induces the selective induction of CTL. The data suggest that B7-1 plasmids should be coadministered with naked DNA vaccines that aim to induce tumor-specific cellular immunity.

  • Copyright © 1997 by American Association of Immunologists

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The Journal of Immunology
Vol. 159, Issue 10
15 Nov 1997
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Costimulation provided by DNA immunization enhances antitumor immunity.
M Corr, H Tighe, D Lee, J Dudler, M Trieu, D C Brinson, D A Carson
The Journal of Immunology November 15, 1997, 159 (10) 4999-5004;

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Costimulation provided by DNA immunization enhances antitumor immunity.
M Corr, H Tighe, D Lee, J Dudler, M Trieu, D C Brinson, D A Carson
The Journal of Immunology November 15, 1997, 159 (10) 4999-5004;
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Print ISSN 0022-1767        Online ISSN 1550-6606