PLoS Pathogens (Oct 2013)

IL-4Rα-associated antigen processing by B cells promotes immunity in Nippostrongylus brasiliensis infection.

  • William G C Horsnell,
  • Matthew G Darby,
  • Jennifer C Hoving,
  • Natalie Nieuwenhuizen,
  • Henry J McSorley,
  • Hlumani Ndlovu,
  • Saeeda Bobat,
  • Matti Kimberg,
  • Frank Kirstein,
  • Anthony J Cutler,
  • Benjamin Dewals,
  • Adam F Cunningham,
  • Frank Brombacher

DOI
https://doi.org/10.1371/journal.ppat.1003662
Journal volume & issue
Vol. 9, no. 10
p. e1003662

Abstract

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In this study, B cell function in protective T(H)2 immunity against N. brasiliensis infection was investigated. Protection against secondary infection depended on IL-4Rα and IL-13; but not IL-4. Protection did not associate with parasite specific antibody responses. Re-infection of B cell-specific IL-4Rα⁻/⁻ mice resulted in increased worm burdens compared to control mice, despite their equivalent capacity to control primary infection. Impaired protection correlated with reduced lymphocyte IL-13 production and B cell MHC class II and CD86 surface expression. Adoptive transfer of in vivo N. brasiliensis primed IL-4Rα expressing B cells into naïve BALB/c mice, but not IL-4Rα or IL-13 deficient B cells, conferred protection against primary N. brasiliensis infection. This protection required MHC class II compatibility on B cells suggesting cognate interactions by B cells with CD4⁺ T cells were important to co-ordinate immunity. Furthermore, the rapid nature of these protective effects by B cells suggested non-BCR mediated mechanisms, such as via Toll Like Receptors, was involved, and this was supported by transfer experiments using antigen pulsed Myd88⁻/⁻ B cells. These data suggest TLR dependent antigen processing by IL-4Rα-responsive B cells producing IL-13 contribute significantly to CD4⁺ T cell-mediated protective immunity against N. brasiliensis infection.