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Infection and Immunity, July 2002, p. 3493-3499, Vol. 70, No. 7
0019-9567/02/$04.00+0 DOI: 10.1128/IAI.70.7.3493-3499.2002
Copyright © 2002, American Society for Microbiology. All Rights Reserved.
Persistence of Protective Immunity to Malaria Induced by DNA Priming and Poxvirus Boosting: Characterization of Effector and Memory CD8+-T-Cell Populations
Martha Sedegah,1,2* Gary T. Brice,1 William O. Rogers,1,
Denise L. Doolan,1,3 Yupin Charoenvit,1 Trevor R. Jones,1 Victoria F. Majam,1 Arnel Belmonte,1 Minh Lu,1 Maria Belmonte,1 Daniel J. Carucci,1 and Stephen L. Hoffman1,
Malaria Program, Naval Medical Research Center, Silver Spring, Maryland 20910-7500,1 Department of Microbiology, The University of Maryland School of Medicine, Baltimore, Maryland 21201-1559,2 Department of Molecular Microbiology and Immunology, School of Hygiene and Public Health, Johns Hopkins University, Baltimore, Maryland 21205-21793
Received 11 December 2001/ Returned for modification 9 January 2002/ Accepted 10 April 2002
The persistence of immunity to malaria induced in mice by a heterologous DNA priming and poxvirus boosting regimen was characterized. Mice were immunized by priming with DNA vaccine plasmids encoding the Plasmodium yoelii circumsporozoite protein (PyCSP) and murine granulocyte-macrophage colony-stimulating factor and boosting with recombinant vaccinia encoding PyCSP. BALB/c mice immunized with either high-dose (100 µg of p PyCSP plus 30 µg of pGM-CSF) or low-dose (1 µg of p PyCSP plus 1 µg of pGM-CSF DNA) priming were protected against challenge with 50 P. yoelii sporozoites. Protection 2 weeks after immunization was 70 to 100%, persisted at this level for at least 20 weeks, and declined to 30 to 40% by 28 weeks. Eight of eight mice protected at 20 weeks were still protected when rechallenged at 40 weeks. The antigen (Ag)-specific effector CD8+-T-cell population present 2 weeks after boosting had ex vivo Ag-specific cytolytic activity, expressed both gamma interferon (IFN-
) and tumor necrosis factor alpha, and constituted 12 to 20% of splenic CD8+ T cells. In contrast, the memory CD8+-Ag-specific-cell population at 28 weeks lacked cytolytic activity and constituted only 6% of splenic CD8+ T cells, but at the single-cell level it produced significantly higher levels of IFN- than the effectors. High levels of Ag- or parasite-specific antibodies present 2 weeks after boosting had declined three- to sevenfold by 28 weeks. Low-dose priming was similarly immunogenic and as protective as high-dose priming against a 50-, but not a 250-, sporozoite challenge. These results demonstrate that a heterologous priming and boosting vaccination can provide lasting protection against malaria in this model system.
* Corresponding author. Mailing address: Malaria Program, Naval Medical Research Center, 503 Robert Grant Ave., Silver Spring, MD 20910-7500. Phone: (301) 319-7586. Fax: (301) 319-7545. E-mail: sedegahm{at}nmrc.navy.mil.
Present address: Naval Medical Research Unit 3, Ghana Detachment, c/o Department of State, Washington, DC 20521-2020.
Present address: Celera Genomics, Rockville, MD 20850.
Infection and Immunity, July 2002, p. 3493-3499, Vol. 70, No. 7
0019-9567/02/$04.00+0 DOI: 10.1128/IAI.70.7.3493-3499.2002
Copyright © 2002, American Society for Microbiology. All Rights Reserved.
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