Malaria Journal (Nov 2008)

Alterations on peripheral B cell subsets following an acute uncomplicated clinical malaria infection in children

  • Ng'ang'a Zipporah W,
  • Kiprotich Chelimo,
  • Moormann Ann M,
  • Asito Amolo S,
  • Ploutz-Snyder Robert,
  • Rochford Rosemary

DOI
https://doi.org/10.1186/1475-2875-7-238
Journal volume & issue
Vol. 7, no. 1
p. 238

Abstract

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Abstract Background The effects of Plasmodium falciparum on B-cell homeostasis have not been well characterized. This study investigated whether an episode of acute malaria in young children results in changes in the peripheral B cell phenotype. Methods Using flow-cytofluorimetric analysis, the B cell phenotypes found in the peripheral blood of children aged 2–5 years were characterized during an episode of acute uncomplicated clinical malaria and four weeks post-recovery and in healthy age-matched controls. Results There was a significant decrease in CD19+ B lymphocytes during acute malaria. Characterization of the CD19+ B cell subsets in the peripheral blood based on expression of IgD and CD38 revealed a significant decrease in the numbers of naive 1 CD38-IgD+ B cells while there was an increase in CD38+IgD- memory 3 B cells during acute malaria. Further analysis of the peripheral B cell phenotype also identified an expansion of transitional CD10+CD19+ B cells in children following an episode of acute malaria with up to 25% of total CD19+ B cell pool residing in this subset. Conclusion Children experiencing an episode of acute uncomplicated clinical malaria experienced profound disturbances in B cell homeostasis.