Background: The cytokine cascade in the immunopathogenesis of malaria infection had been widely studied.
However, their specific association with survival and severe infection remained obscure.
Methods: The study investigated the cytokine profiles and histopathological features of malaria in the severe
infection and survival models by using male ICR mice and male Sprague Dawley rats respectively.
Results: The severe model, the infected ICR mice, exhibited a high parasitemia with 100% mortality after
peak parasitemia at day 5 post-infection. The survival model, the infected Sprague Dawley rats, showed
mild parasitemia with full recovery by day 14 of infection. Both severe and survival models showed similar
histopathological severity during peak parasitemia. The severe model produced highly elevated levels of proinflammatory
cytokines, TNF-α and IL-1α, and low levels of the anti-inflammatory cytokine, IL-4; while the
survival model showed low levels of TNF-α and IL-1α with high levels of IL-4.
Conclusion: There were differences in the pathogenesis of the severe and survival models of malaria infection.
These could be a basis for immunotherapy of malaria in the future.