Characterization of Turbo, a TLR Ligand-based Adjuvant for Glycoconjugate Vaccines
Kishore R. Alugupalli

TL;DR
A new adjuvant called Turbo improves vaccine effectiveness by boosting antibody responses without causing harmful side effects.
Contribution
Turbo, a TLR ligand-based adjuvant, enhances glycoconjugate vaccine immunogenicity across all ages and eliminates the need for boosters.
Findings
Turbo promotes antibody class switching to all IgG isotypes with durable responses and long-lived plasma cells.
Turbo's adjuvanticity is MyD88-dependent and does not rely on inflammasome activation or pyroptotic cell death.
Turbo formulations with TLR ligands improve antibody responses against various bacterial pathogens.
Abstract
Many bacterial polysaccharide vaccines, including the typhoid Vi polysaccharide (ViPS) and tetravalent meningococcal polysaccharide conjugate (MCV4) vaccines, do not incorporate adjuvants and are not highly immunogenic, particularly in infants. I found that endotoxin, a TLR4 ligand in ViPS, contributes to the immunogenicity of typhoid vaccines. Because endotoxin is pyrogenic, and its levels are highly variable in vaccines, I developed monophosphoryl lipid A, a nontoxic TLR4 ligand–based adjuvant named Turbo. Admixing Turbo with ViPS and MCV4 vaccines improved their immunogenicity across all ages and eliminated booster requirement. To understand the characteristics of this adjuvanticity, I compared Turbo with alum. Unlike alum, which polarizes the response toward the IgG1 isotype, Turbo promoted Ab class switching to all IgG isotypes with affinity maturation; the magnitude of this IgG…
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Taxonomy
TopicsImmune Response and Inflammation · Inflammasome and immune disorders · Pneumonia and Respiratory Infections
