Abstract
Human vaccines have used aluminium-based adjuvants (alum) for >80 years despite incomplete understanding of how alum enhances the immune response. Alum can induce the release of endogenous danger signals via cellular necrosis which elicits inflammation-associated cytokines resulting in humoral immunity. IL-33 is proposed to be one such danger signal that is released from necrotic cells. Therefore, we investigated whether there is a role for IL-33 in the adjuvant activity of alum. We show that alum-induced cellular necrosis results in elevated levels of IL-33 following injection in vivo. Alum and IL-33 induce similar increases in IL-5, KC, MCP-1, MIP-1α and MIP-1β; many of which are dependent on IL-33 as shown in IL-33 knockout mice or by using an IL-33-neutralizing recombinant ST2 receptor. Furthermore, IL-33 itself functions as an adjuvant that, while only inducing a marginal primary response, facilitates a robust secondary response comparable to that observed with alum. However, IL-33 is not absolutely required for alum-induced antibody responses since alum mediates similar humoral responses in IL-33 knockout and wild-type mice. Our results provide novel insights into the mechanism of action behind alum-induced cytokine responses and show that IL-33 is sufficient to provide a robust secondary antibody response independently of alum.
Highlights
Response[15,16,17,18]
It has been reported that alum induces cellular necrosis and release of DNA following intraperitoneal (i.p.) injection[19], and IL-33 is proposed to be released from necrotic cells as well[22,27,28]
Since we showed that IL-33 only recapitulates parts of the effects induced by alum, we tested whether co-injection of mouse genomic DNA with IL-33/NP-CGG would result in antibody response profiles that were similar to alum-induced responses
Summary
Response[15,16,17,18]. It was shown that alum-induced cytotoxicity resulted in the release of host DNA that partially mediated the adjuvant activity of alum by enhancing antigen presentation[19,20]. BALB/c mice immunized with IL-33 as the adjuvant showed a similar antibody response kinetic and magnitude for NP-specific IgG1 titers (Fig. 4b) as was observed for C57BL/6 mice (Fig. 4a).
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