Cytotoxic T Cell-Derived Granzyme B Is Increased in Severe Plasmodium Falciparum Malaria

In malaria, CD8 T cells play a double-edged role. Liver-stage specific CD8 T cells can confer protection, as has been shown in several vaccine studies. Blood-stage specific CD8 T cells, on the other hand, contribute to the development of cerebral malaria in murine models of malaria. The role of CD8 T cells in humans during the blood-stage of remains unclear. As part of a cross-sectional malaria study in Ghana, granzyme B levels and CD8 T cells phenotypes were compared in the peripheral blood of children with complicated malaria, uncomplicated malaria, afebrile but asymptomatically infected children and non-infected children. Granzyme B levels in the plasma were significantly higher in children with febrile malaria than in afebrile children. CD8 T cells were the main T cell subset expressing granzyme B. The proportion of granzyme B CD8 T cells was significantly higher in children with complicated malaria than in uncomplicated malaria, whereas the activation marker CD38 on CD8 T cells showed similar expression levels. This suggests a pathogenic role of cytotoxic CD8 T cells in the development of malaria complications in humans.