| Literature DB >> 33177181 |
Laurane De Mot1, Viviane Bechtold1, Vanesa Bol1, Andrea Callegaro1, Margherita Coccia1, Ahmed Essaghir1, Dicle Hasdemir2,3, Fernando Ulloa-Montoya1, Emilio Siena4, Age Smilde3, Robert A van den Berg5, Arnaud M Didierlaurent1, Wivine Burny1, Robbert G van der Most6.
Abstract
The current routine use of adjuvants in human vaccines provides a strong incentive to increase our understanding of how adjuvants differ in their ability to stimulate innate immunity and consequently enhance vaccine immunogenicity. Here, we evaluated gene expression profiles in cells from whole blood elicited in naive subjects receiving the hepatitis B surface antigen formulated with different adjuvants. We identified a core innate gene signature emerging 1 day after the second vaccination and that was shared by the recipients of vaccines formulated with adjuvant systems AS01B, AS01E, or AS03. This core signature associated with the magnitude of the hepatitis B surface-specific antibody response and was characterized by positive regulation of genes associated with interferon-related responses or the innate cell compartment and by negative regulation of natural killer cell-associated genes. Analysis at the individual subject level revealed that the higher immunogenicity of AS01B-adjuvanted vaccine was linked to its ability to induce this signature in most vaccinees even after the first vaccination. Therefore, our data suggest that adjuvanticity is not strictly defined by the nature of the receptors or signaling pathways it activates but by the ability of the adjuvant to consistently induce a core inflammatory signature across individuals.Entities:
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Year: 2020 PMID: 33177181 DOI: 10.1126/scitranslmed.aay8618
Source DB: PubMed Journal: Sci Transl Med ISSN: 1946-6234 Impact factor: 17.956