Luca Casettari scite author profile

It is striking that all marketed SARS-CoV-2 vaccines are developed for intramuscular administration designed to produce humoral and cell mediated immune responses, preventing viremia and the COVID-19 syndrome. They have a high degree of efficacy in humans (70-95%) depending on the type of vaccine. However, little protection is provided against viral replication and shedding in the upper airways due to the lack of a local sIgA immune response, indicating a risk of transmission of virus from vaccinated individuals. A range of novel nasal COVID-19 vaccines are in development and preclinical results in non-human primates have shown a promising prevention of replication and shedding of virus due to the induction of mucosal immune response (sIgA) in upper and lower respiratory tracts as well as robust systemic and humoral immune responses. Whether these results will translate to humans remains to be clarified. An IM prime followed by an IN booster vaccination would likely result in a better well-rounded immune response, including prevention (or strong reduction) in viral replication in the upper and lower respiratory tracts.

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Tight junction modulation by chitosan nanoparticles: Comparison with chitosan solution

Vllasaliu

Exposito-Harris

Heras

et al. 2010

International Journal of Pharmaceutics

218

100

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PEGylated chitosan derivatives: Synthesis, characterizations and pharmaceutical applications

Casettari

Vllasaliu

Castagnino

et al. 2012

Progress in Polymer Science

217

106

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Luca Casettari

Chitosan in nasal delivery systems for therapeutic drugs

Nasal vaccination against SARS-CoV-2: Synergistic or alternative to intramuscular vaccines?

Tight junction modulation by chitosan nanoparticles: Comparison with chitosan solution

PEGylated chitosan derivatives: Synthesis, characterizations and pharmaceutical applications

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