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Publication : DNA released from dying host cells mediates aluminum adjuvant activity.

First Author  Marichal T Year  2011
Journal  Nat Med Volume  17
Issue  8 Pages  996-1002
PubMed ID  21765404 Mgi Jnum  J:174513
Mgi Id  MGI:5139921 Doi  10.1038/nm.2403
Citation  Marichal T, et al. (2011) DNA released from dying host cells mediates aluminum adjuvant activity. Nat Med 17(8):996-1002
abstractText  Aluminum-based adjuvants (aluminum salts or alum) are widely used in human vaccination, although their mechanisms of action are poorly understood. Here we report that, in mice, alum causes cell death and the subsequent release of host cell DNA, which acts as a potent endogenous immunostimulatory signal mediating alum adjuvant activity. Furthermore, we propose that host DNA signaling differentially regulates IgE and IgG1 production after alum-adjuvanted immunization. We suggest that, on the one hand, host DNA induces primary B cell responses, including IgG1 production, through interferon response factor 3 (Irf3)-independent mechanisms. On the other hand, we suggest that host DNA also stimulates 'canonical' T helper type 2 (T(H)2) responses, associated with IgE isotype switching and peripheral effector responses, through Irf3-dependent mechanisms. The finding that host DNA released from dying cells acts as a damage-associated molecular pattern that mediates alum adjuvant activity may increase our understanding of the mechanisms of action of current vaccines and help in the design of new adjuvants.
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