Low doses of killed parasite in CpG elicit vigorous CD4+ T cell responses against blood-stage malaria in mice
Alberto Pinzon-Charry, … , James McCarthy, Michael F. Good
Alberto Pinzon-Charry, … , James McCarthy, Michael F. Good
Published July 12, 2010
Citation Information: J Clin Invest. 2010;120(8):2967-2978. https://doi.org/10.1172/JCI39222.
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Research Article Vaccines

Low doses of killed parasite in CpG elicit vigorous CD4+ T cell responses against blood-stage malaria in mice

Abstract

Development of a vaccine that targets blood-stage malaria parasites is imperative if we are to sustainably reduce the morbidity and mortality caused by this infection. Such a vaccine should elicit long-lasting immune responses against conserved determinants in the parasite population. Most blood-stage vaccines, however, induce protective antibodies against surface antigens, which tend to be polymorphic. Cell-mediated responses, on the other hand, offer the theoretical advantage of targeting internal antigens that are more likely to be conserved. Nonetheless, few of the current blood-stage vaccine candidates are able to harness vigorous T cell immunity. Here, we present what we believe to be a novel blood-stage whole-organism vaccine that, by combining low doses of killed parasite with CpG-oligodeoxynucleotide (CpG-ODN) adjuvant, was able to elicit strong and cross-reactive T cell responses in mice. Our data demonstrate that immunization of mice with 1,000 killed parasites in CpG-ODN engendered durable and cross-strain protection by inducing a vigorous response that was dependent on CD4+ T cells, IFN-γ, and nitric oxide. If applicable to humans, this approach should facilitate the generation of robust, cross-reactive T cell responses against malaria as well as antigen availability for vaccine manufacture.

Authors

Alberto Pinzon-Charry, Virginia McPhun, Vivian Kienzle, Chakrit Hirunpetcharat, Christian Engwerda, James McCarthy, Michael F. Good

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Figure 6

Homologous immunity.

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Homologous immunity. To assess for homologous protection against P. yoel...
To assess for homologous protection against P. yoelii YM, different strains of mice including A/J, B6 and BALB/c mice were immunized with 103 (YM) prbc in CpG-ODN and challenged i.v. with homologous parasites at 2 weeks after vaccination. The outcome of infection was monitored by assessing parasitemia. In all data sets, results for individual mice are shown and are representative of 3 independent experiments performed. Animals that succumbed to infection.