Accelerated CD8+ T-cell memory and prime-boost response after dendritic-cell vaccination

被引:0
作者
Vladimir P Badovinac
Kelly A N Messingham
Ali Jabbari
Jodie S Haring
John T Harty
机构
[1] 3-512 Bowen Science Building,Department of Microbiology
[2] 51 Newton Road,undefined
[3] University of Iowa,undefined
[4] Interdisciplinary Graduate Program in Immunology,undefined
[5] University of Iowa,undefined
[6] 1190 Medical Laboratories,undefined
来源
Nature Medicine | 2005年 / 11卷
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摘要
Efficient boosting of memory T-cell numbers to protective levels generally requires a relatively long interval between immunizations. Decreasing this interval could be crucial in biodefense and cancer immunotherapy, in which rapid protective responses are essential. Here, we show that vaccination with peptide-coated dendritic cells (DCs) generated CD8+ T cells with the phenotype and function of memory cells within 4–6 d. These early memory CD8+ T cells underwent vigorous secondary expansion in response to a variety of booster immunizations, leading to elevated numbers of effector and memory T cells and enhanced protective immunity. Coinjection of CpG oligodeoxynucleotides, potent inducers of inflammation that did not alter the duration of DC antigen display, prevented the rapid generation of memory T cells in wild-type mice but not in mice lacking the interferon (IFN)-γ receptor. These data show that DC vaccination stimulates a pathway of accelerated generation of memory T cells, and suggest that events of inflammation, including the action of IFN-γ on the responding T cells, control the rate of development of memory CD8+ T cells.
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页码:748 / 756
页数:8
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