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Infect. Immun., 05 1997, 1593-1598, Vol 65, No. 5
JB De Souza, KH Williamson, T Otani and JH Playfair
This study was undertaken to explore early differences in cytokine
production during nonlethal and lethal blood-stage murine malaria
infections. Cytokine analysis of spleens during these infections showed
that the principal difference between two nonlethal and two lethal
Plasmodium species was the production of gamma interferon 24 h after
infection with nonlethal parasites. In contrast, no increases in
interleukin-4 production were observed in the first 24 h and tumor necrosis
factor alpha levels increased equally in both nonlethal and lethal
infections. During the later phase of infection with nonlethal parasites,
both gamma interferon and interleukin-4 levels increased markedly a few
days before parasite clearance. Early increases in gamma interferon
production in nonlethal infections of Plasmodium yoelii and Plasmodium
chabaudi were dose related and increased significantly with the size of the
inoculum. Studies with the nonlethal P. yoelii suggest that the early gamma
interferon response is mediated by T cells and natural killer cells, as it
was reduced in athymic mice and in mice depleted of their natural killer
cells by treatment with specific antiserum. Infecting mice with increasing
numbers of lethal P. yoelii and Plasmodium berghei parasites did not
increase the amount of gamma interferon, interleukin-4, and tumor necrosis
factor alpha produced in a dose-dependent fashion. We conclude that one
consequence of the early production of gamma interferon and tumor necrosis
factor-alpha, particularly after nonlethal P. yoelii infection, may be to
adjust the balance of T-helper cell subset activation, and probably that of
other immune responses, so as to enhance the mechanisms that are essential
for elimination of the parasites. This suggests that a successful vaccine
should contain antigens capable of inducing such responses.
Copyright © 1997, American Society for Microbiology
Early gamma interferon responses in lethal and nonlethal murine blood- stage malaria
Department of Immunology, University College London Medical School, United Kingdom.
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