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      Pre-erythrocytic-stage immune effector mechanisms in Plasmodium spp. infections.

      Philosophical Transactions of the Royal Society B: Biological Sciences
      Animals, Plasmodium, immunology, parasitology, Humans, Erythrocytes, physiology, Malaria, Mice, pathogenicity, Malaria Vaccines

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          Abstract

          The potent protective immunity against malaria induced by immunization of mice and humans with radiation-attenuated Plasmodium spp. sporozoites is thought to be mediated primarily by T-cell responses directed against infected hepatocytes. This has led to considerable efforts to develop subunit vaccines that duplicate this protective immunity, but a universally effective vaccine is still not available and in vitro correlates of protective immunity have not been established. Contributing to this delay has been a lack of understanding of the mechanisms responsible for the protection. There are now data indicating that CD8+ T cells, CD4+ T cells, cytokines, and nitric oxide can all mediate the elimination of infected hepatocytes in vitro and in vivo. By dissecting the protection induced by immunization with irradiated sporozoite, DNA and synthetic peptide-adjuvant vaccines, we have demonstrated that different T-cell-dependent immune responses mediate protective immunity in the same inbred strain of mouse, depending on the method of immunization. Furthermore, the mechanism of protection induced by a single method of immunization may vary among different strains of mice. These data have important implications for the development of pre-erythrocytic-stage vaccines designed to protect a heterogeneous human population, and of assays that predict protective immunity.

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          Author and article information

          Journal
          10.1098/rstb.1997.0121
          1692030
          9355128

          Chemistry
          Animals,Plasmodium,immunology,parasitology,Humans,Erythrocytes,physiology,Malaria,Mice,pathogenicity,Malaria Vaccines

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