2021
DOI: 10.1101/2021.07.06.451353
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Receptor-binding domain recombinant protein on alum-CpG induces broad protection against SARS-CoV-2 variants of concern

Abstract: We conducted preclinical studies in mice using a yeast-produced SARS-CoV-2 RBD219-N1C1 subunit vaccine candidate formulated with aluminum hydroxide (alum) and CpG deoxynucleotides. This vaccine formulation is similar to one that entered advanced phase 3 clinical development in India. We compared the immune response of mice vaccinated with RBD219-N1C1/alum to mice vaccinated with RBD219-N1C1/alum+CpG. We also evaluated mice immunized with RBD219-N1C1/alum+CpG and boosted with RBD219-N1C1/alum. Mice were immuniz… Show more

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Cited by 8 publications
(5 citation statements)
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“…In this study, these titres were higher than obtained with the NIBSC 20/136 reference control and those elicited by a DNA vaccine encoding whole S protein, which was also reflected in the ACE2 binding inhibition assay, suggesting that vaccination with RBD may elicit higher neutralising antibody titres than vaccination with the complete S antigen. Despite the fact that this may be linked to the protein expression levels from the vaccines in this study, these findings are concordant with other studies in mice in which the whole S protein or an RBD trimer have been delivered as recombinant protein, RNA or adenovirus vectors in prime boost regimes 19,4651 . Our in vivo efficacy data demonstrate that the antibody titres and T cell responses induced were sufficient to protect mice from lethal viral challenge and promote survival.…”
Section: Discussionsupporting
confidence: 92%
“…In this study, these titres were higher than obtained with the NIBSC 20/136 reference control and those elicited by a DNA vaccine encoding whole S protein, which was also reflected in the ACE2 binding inhibition assay, suggesting that vaccination with RBD may elicit higher neutralising antibody titres than vaccination with the complete S antigen. Despite the fact that this may be linked to the protein expression levels from the vaccines in this study, these findings are concordant with other studies in mice in which the whole S protein or an RBD trimer have been delivered as recombinant protein, RNA or adenovirus vectors in prime boost regimes 19,4651 . Our in vivo efficacy data demonstrate that the antibody titres and T cell responses induced were sufficient to protect mice from lethal viral challenge and promote survival.…”
Section: Discussionsupporting
confidence: 92%
“…When the COVID-19 genome was made available in January 2020, Texas Children's CVD coronavirus vaccine program pivoted to this new virus, and a prototype vaccine was developed and successfully tested including in a non-human primate virus challenge model [26]. Each step in the vaccine development process was published in the open access biomedical literature available on the PubMed National Library of Medicine database [27][28][29][30][31]. Baylor College of Medicine then non-exclusively licensed the vaccine technology on favorable terms and without patent protection to several LMIC vaccine producers.…”
Section: A Valuable Covid-19 Vaccine Development Model-technological ...mentioning
confidence: 99%
“…The RBD attaches to ACE-2 in human cells mediating infection (Tai et al, 2020). Compared to the RBD219-N1C1, RBD203-N1 was found to have increased production yields while maintaining equivalent biophysical and immunological properties (Chen et al, 2022;Pollet et al, 2022). The immunogenicity of this family of RBD antigens has primarily been tested using Alum as an adjuvant and formulation system, with or without the addition of either the TLR9 agonist CpG-1018 or the TLR7/8 agonist 3M-052 (Chen et al, 2020;Pino et al, 2021;Pollet et al, 2022).…”
Section: Introductionmentioning
confidence: 99%
“…Compared to the RBD219-N1C1, RBD203-N1 was found to have increased production yields while maintaining equivalent biophysical and immunological properties (Chen et al, 2022;Pollet et al, 2022). The immunogenicity of this family of RBD antigens has primarily been tested using Alum as an adjuvant and formulation system, with or without the addition of either the TLR9 agonist CpG-1018 or the TLR7/8 agonist 3M-052 (Chen et al, 2020;Pino et al, 2021;Pollet et al, 2022). It is of interest to understand how RBD203-N1 (hereafter RBD) interacts with other common adjuvant formulations and agonists, such as squalene emulsions, the synthetic TLR4 agonist glucopyranosyl lipid adjuvant (GLA), the murine TLR9 agonist CpG-1826 (CpG), the TLR7/8 agonist 3M-052, and the detoxified Escherichia coli double mutant heat-labile toxin (dmLT) LT(R192G/L211A), all of which are in either clinical or commercial stage use, to determine if there are synergies, or how these formulations influence the immune phenotype of the RBD vaccine.…”
Section: Introductionmentioning
confidence: 99%