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Emulsion adjuvant-induced uric acid release modulates optimal immunogenicity by targeting dendritic cells and B cells

Authors
 Lee, Sun Min  ;  Lee, Junghwa  ;  Kim, Dong-In  ;  Avila, Jonathan P.  ;  Nakaya, Helder  ;  Kwak, Kihyuck  ;  Kim, Eui Ho 
Citation
 NPJ VACCINES, Vol.10(1), 2025-04 
Article Number
 72 
Journal Title
NPJ VACCINES
ISSN
 2059-0105 
Issue Date
2025-04
Keywords
Squalene ; Uric Acid ; Cytokine ; Influenza Vaccine ; Squalene ; Uric Acid ; Adaptive Immunity ; Animal Cell ; Animal Experiment ; Animal Model ; Antigen Presentation ; Article ; B Lymphocyte ; B Lymphocyte Activation ; Cell Proliferation ; Cellular Immunity ; Controlled Study ; Crystal ; Damage-associated Molecular Pattern-triggered Immunity ; Dendritic Cell ; Draining Lymph Node ; Emulsion ; Female ; Humoral Immunity ; Immunogenicity ; In Vitro Study ; In Vivo Study ; Influenza ; Innate Immunity ; Mouse ; Nonhuman ; Protection ; Synthesis ; T Lymphocyte ; Vaccination
Abstract
Squalene-based emulsion (SE) adjuvants like MF59 and AS03 are used in protein subunit vaccines against influenza virus (e.g., Fluad, Pandemrix, Arepanrix) and SARS-CoV-2 (e.g., Covifenz, SKYCovione). We demonstrate the critical role of uric acid (UA), a damage-associated molecular pattern (DAMP), in triggering immunogenicity by SE adjuvants. In mice, SE adjuvants elevated DAMP levels in draining lymph nodes. Strikingly, inhibition of UA synthesis reduced vaccine-induced innate immunity, subsequently impairing optimal antibody and T cell responses. In vivo treatment with UA crystals elicited partial adjuvant effects. In vitro stimulation with UA crystals augmented the activation of dendritic cells (DCs) and B cells and altered multiple pathways in these cells, including inflammation and antigen presentation in DCs and cell proliferation in B cells. In an influenza vaccine model, UA contributed to protection against influenza viral infection. These results demonstrate the importance of DAMPs, specifically the versatile role of UA in the immunogenicity of SE adjuvants, by regulating DCs and B cells.
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DOI
10.1038/s41541-025-01130-z
Appears in Collections:
1. College of Medicine (의과대학) > Dept. of Microbiology (미생물학교실) > 1. Journal Papers
Yonsei Authors
Kwak, Kihyuck(곽기혁)
URI
https://ir.ymlib.yonsei.ac.kr/handle/22282913/208628
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