Evidence for Multiple B- and T-Cell Epitopes in
Plasmodium falciparum
Liver-Stage Antigen 3
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Published:2009-03
Issue:3
Volume:77
Page:1189-1196
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ISSN:0019-9567
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Container-title:Infection and Immunity
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language:en
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Short-container-title:Infect Immun
Author:
Toure-Balde Aissatou1, Perlaza Blanca-Liliana2, Sauzet Jean-Pierre2, Ndiaye Mouhamadou1, Aribot Georgette1, Tall Adama1, Sokhna Cheikh3, Rogier Christophe4, Corradin Giampietro5, Roussilhon Christian2, Druilhe Pierre2
Affiliation:
1. Institut Pasteur de Dakar, Dakar, Senegal 2. Bio-Medical Parasitology Unit, Institut Pasteur, Paris, France 3. Institut de Recherche et de Developpement, Dakar, Senegal 4. Institut de Medecine Tropicale du Service de Sante des Armees, Marseille, France 5. Institute of Biochemistry, University of Lausanne, Lausanne, Switzerland
Abstract
ABSTRACT
Liver-stage antigen 3 (LSA-3) is a new vaccine candidate that can induce protection against
Plasmodium falciparum
sporozoite challenge. Using a series of long synthetic peptides (LSP) encompassing most of the 210-kDa LSA-3 protein, a study of the antigenicity of this protein was carried out in 203 inhabitants from the villages of Dielmo (
n
= 143) and Ndiop (
n
= 60) in Senegal (the level of malaria transmission differs in these two villages). Lymphocyte responses to each individual LSA-3 peptide were recorded, some at high prevalences (up to 43%). Antibodies were also detected to each of the 20 peptides, many at high prevalence (up to 84% of responders), and were directed to both nonrepeat and repeat regions. Immune responses to LSA-3 were detectable even in individuals of less than 5 years of age and increased with age and hence exposure to malaria, although they were not directly related to the level of malaria transmission. Thus, several valuable T- and B-cell epitopes were characterized all along the LSA-3 protein, supporting the antigenicity of this
P. falciparum
vaccine candidate. Finally, antibodies specific for peptide LSP10 located in a nonrepeat region of LSA-3 were found significantly associated with a lower risk of malaria attack over 1 year of daily clinical follow-up in children between the ages of 7 and 15 years, but not in older individuals.
Publisher
American Society for Microbiology
Subject
Infectious Diseases,Immunology,Microbiology,Parasitology
Reference34 articles.
1. BenMohamed, L., H. Gras-Masse, A. Tartar, P. Daubersies, K. Brahimi, M. Bossus, A. Thomas, and P. Druilhe. 1997. Lipopeptide immunization without adjuvant induces potent and long-lasting B, T-helper, and cytotoxic T lymphocyte responses against a malaria liver stage antigen in mice and chimpanzees. Eur. J. Immunol.27:1242-1253. 2. Human Antibodies against
Plasmodium falciparum
Liver-Stage Antigen 3 Cross-React with
Plasmodium yoelii
Preerythrocytic-Stage Epitopes and Inhibit Sporozoite Invasion In Vitro and In Vivo 3. Dame, J. B., J. L. Williams, T. F. McCutchan, J. L. Weber, R. A. Wirtz, W. T. Hockmeyer, W. L. Maloy, J. D. Haynes, I. Schneider, D. Roberts, et al. 1984. Structure of the gene encoding the immunodominant surface antigen on the sporozoite of the human malaria parasite Plasmodium falciparum. Science225:593-599. 4. Daubersies, P., A. W. Thomas, P. Millet, K. Brahimi, J. A. Langermans, B. Ollomo, L. BenMohamed, B. Slierendregt, W. Eling, A. Van Belkum, G. Dubreuil, J. F. Meis, C. Guerin-Marchand, S. Cayphas, J. Cohen, H. Gras-Masse, P. Druilhe, and L. B. Mohamed. 2000. Protection against Plasmodium falciparum malaria in chimpanzees by immunization with the conserved pre-erythrocytic liver-stage antigen 3. Nat. Med.6:1258-1263. 5. Del Giudice, G., Q. Cheng, D. Mazier, N. Berbiguier, J. A. Cooper, H. D. Engers, C. Chizzolini, A. S. Verdini, F. Bonelli, A. Pessi, et al. 1988. Immunogenicity of a non-repetitive sequence of Plasmodium falciparum circumsporozoite protein in man and mice. Immunology63:187-191.
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