| Literature DB >> 28748530 |
I Sebina1,2, L G Fogg1, K R James1,2, M S F Soon1,2, J Akter1,2, B S Thomas1, G R Hill1, C R Engwerda1, A Haque1.
Abstract
Humoral immunity develops in the spleen during blood-stage Plasmodium infection. This elicits parasite-specific IgM and IgG, which control parasites and protect against malaria. Studies in mice have elucidated cells and molecules driving humoral immunity to Plasmodium, including CD4+ T cells, B cells, interleukin (IL)-21 and ICOS. IL-6, a cytokine readily detected in Plasmodium-infected mice and humans, is recognized in other systems as a driver of humoral immunity. Here, we examined the effect of infection-induced IL-6 on humoral immunity to Plasmodium. Using P. chabaudi chabaudi AS (PcAS) infection of wild-type and IL-6-/- mice, we found that IL-6 helped to control parasites during primary infection. IL-6 promoted early production of parasite-specific IgM but not IgG. Notably, splenic CD138+ plasmablast development was more dependent on IL-6 than germinal centre (GC) B-cell differentiation. IL-6 also promoted ICOS expression by CD4+ T cells, as well as their localization close to splenic B cells, but was not required for early Tfh-cell development. Finally, IL-6 promoted parasite control, IgM and IgG production, GC B-cell development and ICOS expression by Tfh cells in a second model, Py17XNL infection. IL-6 promotes CD4+ T-cell activation and B-cell responses during blood-stage Plasmodium infection, which encourages parasite-specific antibody production.Entities:
Keywords: B lymphocyte; CD4 T lymphocyte; animal model; costimulatory molecules; cytokine; humoral immunity; malaria
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Year: 2017 PMID: 28748530 DOI: 10.1111/pim.12455
Source DB: PubMed Journal: Parasite Immunol ISSN: 0141-9838 Impact factor: 2.280