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A comparison of non-toxin vaccine adjuvants for their ability to enhance the immunogenicity of nasally-administered anthrax recombinant protective antigen
Authors:William M Gwinn  Brandi T Johnson  Shaun M Kirwan  Ashley E Sobel  Soman N Abraham  Michael D Gunn  Herman F Staats
Institution:1. Duke University Medical Center, Department of Pathology, Durham, NC 27710, USA;2. Duke University Medical Center, Department of Molecular Genetics and Microbiology, Durham, NC 27710, USA;3. Duke University Medical Center, Department of Immunology, Durham, NC 27710, USA;4. Duke University Medical Center, Department of Medicine, Durham, NC 27710, USA;5. Duke University Medical Center, The Duke Human Vaccine Institute, Durham, NC 27710, USA
Abstract:Development of nasal immunization for human use is hindered by the lack of acceptable adjuvants. Although CT is an effective adjuvant, its toxicity will likely prevent its use in nasal vaccines. This study compared non-toxin adjuvants to CT for their ability to induce protective antibody responses with nasal immunization. C3H/HeN and C57BL/6 mice were immunized with rPA formulated with the following adjuvants: CT, IL-1α, LPS, CpG, Pam3CSK4, 3M-019, resiquimod/R848 or c48/80. Serum and nasal wash cytokine concentrations were monitored 6 h post-vaccination as biomarkers for acute activation of the innate immune system. Not all of the adjuvants induced significant changes in innate serum or nasal wash cytokines, but when changes were observed, the cytokine signatures were unique for each adjuvant. All adjuvants except Pam3CSK4 induced significantly increased anti-rPA serum IgG titers in both strains of mice, while only IL-1α, c48/80 and CpG enhanced mucosal anti-rPA IgA. Pam3CSK4 was the only adjuvant unable to enhance the induction of serum LeTx-neutralizing antibodies in C3H/HeN mice while c48/80 was the only adjuvant to induce increased serum LeTx-neutralizing antibodies in C57BL/6 mice. Only CT enhanced total serum IgE in C3H/HeN mice while IL-1α enhanced total serum IgE in C57BL/6 mice. The adjuvant influenced antigen-specific serum IgG subclass and T cell cytokine profiles, but these responses did not correlate with the induction of LeTx-neutralizing activity. Our results demonstrate the induction of diverse innate and adaptive immune responses by non-toxin nasal vaccine adjuvants that lead to protective humoral immunity comparable to CT and that these responses may be influenced by the host strain.
Keywords:Nasal immunization  Non-toxin adjuvants  Toll-like receptor ligands  Compound 48/80
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