Publication | Open Access
Role of nanoscale antigen organization on B-cell activation probed using DNA origami
30
Citations
38
References
2020
Year
Unknown Venue
Immunocytochemical TechniqueEngineeringImmunologyMolecular BiologyAntigen ProcessingBiomedical EngineeringDna OrigamiImmunotherapyB CellSynthetic ImmunologyNanomedicineDna NanotechnologyDna Origami NanoparticlesNanoscale Antigen OrganizationBiophysicsNanobiotechnologyDna ReplicationTherapeutic VaccineAntigen ValencyCell BiologyAntiviral ResponseVaccine DesignMedicineViral ImmunityB-cell Activation
ABSTRACT Arraying vaccine immunogens in a multivalent form on the surface of virus-like particles is an important strategy used to enhance the efficacy of subunit vaccines. However, the impacts of antigen valency, spacing, and spatial organization on B cell triggering remain poorly understood. Here, we use DNA origami nanoparticles to create precise nanoscale organizations of a clinically-relevant HIV gp120 immunogen to systematically interrogate their impact on B cell triggering in vitro . We find that antigen dimers elicit monotonically increasing B cell receptor activation as inter-antigen spacing increases up to ~30 nm, and only 5 immunogens arrayed on the surface of a 3D particle are needed to elicit maximal B cell calcium signaling. Our results reveal design principles of viral and immunogen display that drive functional B cell responses.
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