Intranasal Multiepitope PD‐L1‐siRNA‐Based Nanovaccine: The Next‐Gen COVID‐19 Immunotherapy

Author:

Acúrcio Rita C.1ORCID,Kleiner Ron2ORCID,Vaskovich‐Koubi Daniella2ORCID,Carreira Bárbara1ORCID,Liubomirski Yulia2,Palma Carolina1,Yeheskel Adva3ORCID,Yeini Eilam2ORCID,Viana Ana S.4,Ferreira Vera1,Araújo Carlos1,Mor Michael5ORCID,Freund Natalia T.5ORCID,Bacharach Eran6ORCID,Gonçalves João1,Toister‐Achituv Mira7,Fabregue Manon8,Matthieu Solene8,Guerry Capucine8,Zarubica Ana8ORCID,Aviel‐Ronen Sarit9ORCID,Florindo Helena F.1ORCID,Satchi‐Fainaro Ronit210ORCID

Affiliation:

1. Research Institute for Medicines (iMed.ULisboa) Faculty of Pharmacy Universidade de Lisboa Lisbon 1649‐003 Portugal

2. Department of Physiology and Pharmacology Faculty of Medicine Tel Aviv University Tel Aviv 6997801 Israel

3. The Blavatnik Center for Drug Discovery Tel Aviv University Tel Aviv 6997801 Israel

4. Center of Chemistry and Biochemistry Faculty of Sciences University of Lisbon Lisbon 1749‐016 Portugal

5. Department of Clinical Microbiology and Immunology Faculty of Medicine Tel Aviv University Tel Aviv 6997801 Israel

6. The Shmunis School of Biomedicine and Cancer Research George S. Wise Faculty of Life Sciences Tel Aviv University Tel Aviv 6997801 Israel

7. Inter‐Lab, a subsidiary of Merck KGaA, South Industrial Area Yavne 8122004 Israel

8. Centre d'Immunophénomique Aix Marseille Université Inserm, CNRS, PHENOMIN Marseille 13284 France

9. Adelson School of Medicine Ariel University Ariel 4070000 Israel

10. Sagol School of Neuroscience Tel Aviv University Tel Aviv 6997801 Israel

Abstract

AbstractThe first approved vaccines for human use against severe acute respiratory syndrome coronavirus 2 (SARS‐CoV‐2) are nanotechnology‐based. Although they are modular, rapidly produced, and can reduce disease severity, the currently available vaccines are restricted in preventing infection, stressing the global demand for novel preventive vaccine technologies. Bearing this in mind, we set out to develop a flexible nanovaccine platform for nasal administration to induce mucosal immunity, which is fundamental for optimal protection against respiratory virus infection. The next‐generation multiepitope nanovaccines co‐deliver immunogenic peptides, selected by an immunoinformatic workflow, along with adjuvants and regulators of the PD‐L1 expression. As a case study, we focused on SARS‐CoV‐2 peptides as relevant antigens to validate the approach. This platform can evoke both local and systemic cellular‐ and humoral‐specific responses against SARS‐CoV‐2. This led to the secretion of immunoglobulin A (IgA), capable of neutralizing SARS‐CoV‐2, including variants of concern, following a heterologous immunization strategy. Considering the limitations of the required cold chain distribution for current nanotechnology‐based vaccines, it is shown that the lyophilized nanovaccine is stable for long‐term at room temperature and retains its in vivo efficacy upon reconstitution. This makes it particularly relevant for developing countries and offers a modular system adaptable to future viral threats.

Funder

European Research Council

Israel Cancer Research Fund

'la Caixa' Foundation

Melanoma Research Alliance

Israel Science Foundation

Fundação para a Ciência e a Tecnologia

Publisher

Wiley

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