Both alum, which is associated with type-2 responses, and CFA, which is in general associated with type-1
immune responses, induced expression of IL-4 mRNA in eosinophils 17, 18. The mechanisms by which adjuvants mediate their effects on the immune system are VX-809 molecular weight only poorly understood and, in particular, their means of activation of eosinophils remain obscure 5, 18. As in vitro LPS activation of sorted eosinophils shows an upregulation of cytokine expression, it is likely that eosinophils are directly activated by the mycobacterial components present in CFA. However, adjuvant effects of alum have been shown to be independent of TLR, and activation by alum is suggested to be regulated through the NALP3 inflammasome 19. Injection of antigen-free alum induced only a transient stimulation of eosinophils, suggesting that antigen-specific priming of the adaptive immune system is required to maintain eosinophils in an activated stage so that, as shown here even
60 days after antigen priming, eosinophils have elevated cytokine expression. Furthermore, in the secondary response, the degree of eosinophil selleck activation was even higher suggesting that antigen-dependent re-activation of the memory immune response accelerates long-term cytokine expression in eosinophils. Immunization of mice not only induces eosinophil activation but also their stable accumulation in the BM. How is that possible, considering the short half life of eosinophils which turn over within a couple of days 20? What are the mechanisms by which long-term changes in the immune compartments are achieved? Mutual interactions between eosinophils and various cell types in the BM micro-environment may contribute to the continuous activation of eosinophils. Activated eosinophils are shown to secrete a broad-spectrum of mediators one of which is the T-cell-activating cytokine IL-4 Morin Hydrate 2, 5. Further experiments
will be required to show whether enhanced levels of IL-4 induce expression of IL-5 in memory T cells which are only found in the BM after immunization with antigen 21. The cytokine IL-5 is a key factor for the development of eosinophils 22. Enhanced levels of IL-5 may affect the generation of eosinophils and, in addition, it may also prolong the life time of eosinophils. In long-term immunized animals, we find that in the network of reticular stromal cells, plasma cells are embedded within clusters of eosinophils 9. As eosinophils express Fc-receptors, Ig secretion by plasma cells may contribute to eosinophil activation, and it also may prolong the life time of eosinophils in the BM 23, 24. Furthermore, the network of stromal reticular cells may add to the activation of eosinophils by enhanced secretion of cytokines.