Severe Plasmodium falciparum malaria is a major cause of global mortality, yet the immunological factors underlying progression to severe disease remain unclear. CD4 + CD25 + regulatory T cells (Treg cells) are associated with impaired T cell control of Plasmodium spp infection. We investigated the relationship between Treg cells, parasite biomass, and P. falciparum malaria disease severity in adults living in a malaria-endemic region of Indonesia. CD4 + CD25 + Foxp3 + CD127 lo Treg cells were significantly elevated in patients with uncomplicated (UM; n = 17) and severe malaria (SM; n = 16) relative to exposed asymptomatic controls (AC; n = 10). In patients with SM, Treg cell frequency correlated positively with parasitemia (r = 0.79, p = 0.0003) and total parasite biomass (r = 0.87, p,0.001), both major determinants for the development of severe and fatal malaria, and Treg cells were significantly increased in hyperparasitemia. There was a further significant correlation between Treg cell frequency and plasma concentrations of soluble tumor necrosis factor receptor II (TNFRII) in SM. A subset of TNFRII + Treg cells with high expression of Foxp3 was increased in severe relative to uncomplicated malaria. In vitro, P. falciparum–infected red blood cells dose dependently induced TNFRII + Foxp3 hi Treg cells in PBMC from malaria-unexposed donors which showed greater suppressive activity than TNFRII - Treg cells. The selective enrichment of the Treg cell compartment for a maximally suppressive TNFRII + Foxp3 hi Treg subset in severe malaria provides a potential link between immune suppression, increased parasite biomass, and malaria disease severity. The findings caution against the induction of TNFRII + Foxp3 hi Treg cells when developing effective malaria vaccines.
CITATION STYLE
Minigo, G., Woodberry, T., Piera, K. A., Salwati, E., Tjitra, E., Kenangalem, E., … Plebanski, M. (2009). Parasite-dependent expansion of TNF receptor ii– positive regulatory T cells with enhanced suppressive activity in adults with severe Malaria. PLoS Pathogens, 5(4). https://doi.org/10.1371/journal.ppat.1000402
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