SARS-CoV-2 XBB.1.5 mRNA booster vaccination elicits limited mucosal immunity

Lasrado, Ninaad; Rowe, Marjorie; McMahan, Katherine; Hachmann, Nicole P.; Miller, Jessica; Jacob-Dolan, Catherine; Liu, Jinyan; Verrette, Brookelynne; Gotthardt, Kristin A.; Ty, Darren M.; Pereira, Juliana; Mazurek, Camille R.; Hoyt, Amelia; Collier, Ai-ris Y.; Barouch, Dan H.

doi:10.1126/scitranslmed.adp8920

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2024

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A Modular Bacteriophage T4 Nanoparticle Platform Enables Rapid Design of Dual COVID-19-Flu Mucosal Vaccines

Zhu,

Sha,

Batra

et al. 2024

Preprint

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A multivalent, rapidly deployable, mucosal vaccine platform is desperately needed to prevent the acquisition and transmission of respiratory infections during epidemics and pandemics. We present one such bacteriophage T4-based platform, and design of dual COVID-19-Flu mucosal vaccines by exploiting its unique architecture. These include: T4's natural affinity for nasal mucosa, flexible engineering to incorporate multiple antigens, and repeat and symmetric epitope presentation for enhanced B cell responses. Hundreds of SARS-CoV-2 spike trimers and nucleocapsid proteins, and influenza hemagglutinin trimers and M2e peptides, were incorporated into a single phage, creating the highest density nanoparticle presentation yet reported. Intranasal administration of adjuvant-free vaccine induced robust mucosal immunity in mice including, neutralizing antibody and secretory IgA, lung-resident CD4+/CD8+ T cells, diverse memory B cells, and complete protection against SARS-CoV-2 and influenza challenges. The noninfectious T4 phage offers an extraordinary platform to rapidly design potent mucosal vaccines against emerging bacterial and viral threats.

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