Structural Design and Immunogenicity of a Novel Self‐Adjuvanting Mucosal Vaccine Candidate for SARS‐CoV‐2 Expressed in Plants
Mi‐Young Kim, Andy Cano Tran, Ju Kim, Humblenoble Stembridge Ayuk, Adam Sparrow, Lorenzo Bossi, Megan Brown, Emil Joseph Vergara, Kathrin Göritzer, Elisabetta Groppelli, Tae‐Ho Kwon, Julian K. C. Ma, Yong‐Suk Jang, Rajko Reljic

TL;DR
A new mucosal vaccine for SARS-CoV-2 was developed using a plant-based system, showing strong immune responses and potential for respiratory delivery.
Contribution
A novel self-adjuvanting mucosal vaccine platform for SARS-CoV-2 was developed using a plant expression system.
Findings
The PCF vaccine induces systemic and mucosal antibodies and lung-resident memory T cells in mice.
The vaccine is recognized by immune cells and forms immune complexes with circulating antibodies.
The vaccine can be aerosolized without losing activity and is non-toxic to human cells.
Abstract
Mucosal vaccination for COVID‐19 to boost preexisting though insufficient systemic and local/mucosal immunity remains an attractive prospect but there are currently no licensed mucosal vaccines against this infection. Here, using a plant expression system, we developed a novel mucosal vaccine platform for respiratory viruses and demonstrated its application in the context of SARS‐CoV‐2 infection. In addition to the antigen itself, the PCF (Platform CTB‐Fc) vaccine candidate incorporates two molecular adjuvants, the IgG‐Fc antibody fragment and the nontoxic cholera toxin B subunit (CTB), with the first targeting the vaccine to IgG receptors on antigen‐presenting cells, and the second providing local adjuvanticity by targeting cellular gangliosides in the mucosae. We demonstrated that this vaccine candidate is highly immunogenic in mice, inducing virus‐neutralising systemic and mucosal…
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Taxonomy
TopicsTransgenic Plants and Applications · SARS-CoV-2 and COVID-19 Research · Toxin Mechanisms and Immunotoxins
