Coordination between T helper cells, iNKT cells, and their follicular helper subsets in the humoral immune response against Clostridium difficiletoxin B

Autor: Rampuria, Pragya, Lang, Gillian A., Devera, T. Scott, Gilmore, Casey, Ballard, Jimmy D., Lang, Mark L.
Zdroj: Journal of Leukocyte Biology; February 2017, Vol. 101 Issue: 2 p567-576, 10p
Abstrakt: Activation of iNKT cells with the CD1d-binding glycolipid adjuvant a-galactosylceramide (a-GC) enhances humoral immunity specific for coadministered T-dependent Ag. However, the relationship between the iNKT cell and the classic T helper (Th) or T follicular helper (Tfh) function following this immunization modality remains unclear. We show that immunization with the C-terminal domain (CTD) of Clostridium difficiletoxin B (TcdB), accompanied by activation of iNKT cells with a-GC, led to enhanced production of CTD-specific IgG, which was CD1d- and iNKT cell-dependent and associated with increased neutralization of active TcdB. Immunization with CTD plus a-GC followed by NP hapten-linked CTD increased NP-specific IgG1 titers in an NKT-dependent manner, suggesting that iNKT activation could enhance Th or Tfh function or that iNKT and iNKTfh cells could provide supplemental, yet independent, B cell help. Th, Tfh, iNKT, and iNKTfh cells were, therefore, examined quantitatively, phenotypically, and functionally following immunization with CTD or with CTD plus a-GC. Our results demonstrated that a-GC–activated iNKT cells had no direct effect on the numbers, phenotype, or function of Th or Tfh cells. However, CD4+T cell–specific ablation of the Bcl6transcription factor demonstrated that Tfh and iNKTfh cells both contributed to B cell help. This work extends our understanding of the immune response to vaccination and demonstrates an important contribution by NKTfh cells to humoral immunity.
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