Evidence Of Functional Cell-Mediated Immune Responses To Nontypeable Haemophilus Influenzae In Otitis-Prone Children

Otitis media (OM) remains a common paediatric disease, despite advances in vaccinology. Susceptibility to recurrent acute OM (rAOM) has been postulated to involve defective cell-mediated immune responses to common otopathogenic bacteria. We compared the composition of peripheral blood mononuclear cells (PBMC) from 20 children with a history of rAOM (otitis-prone) and 20 healthy non-otitis-prone controls, and assessed innate and cell-mediated immune responses to the major otopathogen nontypeable Haemophilus influenzae (NTHi). NTHi was a potent stimulator of inflammatory cytokine secretion from PBMC within 4 hours, with no difference in cytokine levels produced between PBMC from cases or controls. In the absence of antigen stimulation, otitis-prone children had more circulating Natural Killer (NK) cells (p<0.01), particularly NKdim (CD56(lo)) cells (p<0.01), but fewer CD4(+) T cells (p<0.01) than healthy controls. NTHi challenge significantly increased the proportion of activated (CD107a(+)) NK cells in otitis-prone and non-otitis-prone children (p<0.01), suggesting that NK cells from otitis-prone children are functional and respond to NTHi. CD8(+) T cells and NK cells from both cases and controls produced IFN gamma in response to polyclonal stimulus (Staphylococcal enterotoxin B; SEB), with more IFN gamma(+) CD8(+) T cells present in cases than controls (p<0.05) but similar proportions of IFN gamma(+) NK cells. Otitis prone children had more circulating IFN gamma-producing NK cells (p<0.05) and more IFN gamma-producing CD4(+) (p<0.01) or CD8(+) T-cells (p<0.05) than healthy controls. In response to SEB, more CD107a-expressing CD8(+) T cells were present in cases than controls (p<0.01). Despite differences in PBMC composition, PBMC from otitis-prone children mounted innate and T cell-mediated responses to NTHi challenge that were comparable to healthy children. These data provide evidence that otitis-prone children do not have impaired functional cell mediated immunity.