A randomized, double-blind phase I clinical trial of two recombinant dimeric RBD COVID-19 vaccine candidates: safety, reactogenicity and immunogenicity

Abstract: Background The Receptor Binding Domain (RBD) of the SARS-CoV-2 spike protein is the target for many COVID-19 vaccines. Here we report results for phase 1 clinical trial of two COVID-19 vaccine candidates based on recombinant dimeric RBD (d-RBD). Methods We performed a randomized, double-blind, phase I clinical trial in the National Centre of Toxicology in Havana. Sixty Cuban volunteers aged 19-59 years were randomized into three groups (20 subjects each): 1) FINLAY-FR-1 (50 mcg d-RBD plus outer membrane vesicl… Show more

“…In humans, the formulation containing the OMVs elicits a more potent neutralizing effect against RBD mutants present in VOCs, including the triple-mutant RBD of the beta variant. These results, together with those of phase I clinical trial, 40 pave the way for phase II and III clinical trials for the RBD-d/OMV/alum formulation. They also demonstrate the advantages of using N. meningitidis OMVs not only in antibacterial vaccines, but also as adjuvants in antiviral protein subunit vaccines.…”

“…19 Human immunogenicity A phase I clinical trial was conducted to compare these and other vaccine candidates, in groups of 20 subjects following a three-dose schedule at intervals of 28 days. 39 While the safety, reactogenicity and immunogenicity were reported, 40 here we describe additional results which enable to further assess the effect of OMVs on the quality of the antibody response in humans. The analysis was performed with sera from trial participants vaccinated with RBD-d/ OMV/alum (50 mg/20 mg/1250 mg) and RBD-d/alum (50 mg/1250 mg).…”

“…The number of subjects with IgG concentration 470 AU/mL increased after the third dose with respect to the second one: for RBD-d/OMV/alum from 13/20 (65%) to 18/20 (90%) and for RBD-d/alum from 10/20 (50%) to 13/20 (65%). 40 Interestingly, while the IgG response at day 28 after the second (T = 56) and third doses (T = 84) was rather similar, 40 the quality of the IgG response was certainly higher for both formulations on day 28 after the third vaccination (T = 84), as determined by the inhibition of the RBD-ACE2 interaction. In mVNT 50 , the percentage of subjects attaining an ID 50 4 150 comparing the inhibition of the interaction between the phage-displayed RBD mutants and the ACE2 receptor.…”

“…Fig.4Immunogenicity evaluation from a phase I clinical trial 39,40. Subjects immunized with RBD-d/OMV (50 mg/20 mg, blue) vs. RBD-d (50 mg, red) adsorbed in alum.…”

A COVID-19 vaccine candidate composed of the SARS-CoV-2 RBD dimer and Neisseria meningitidis outer membrane vesicles

“…In humans, the formulation containing the OMVs elicits a more potent neutralizing effect against RBD mutants present in VOCs, including the triple-mutant RBD of the beta variant. These results, together with those of phase I clinical trial, 40 pave the way for phase II and III clinical trials for the RBD-d/OMV/alum formulation. They also demonstrate the advantages of using N. meningitidis OMVs not only in antibacterial vaccines, but also as adjuvants in antiviral protein subunit vaccines.…”

“…19 Human immunogenicity A phase I clinical trial was conducted to compare these and other vaccine candidates, in groups of 20 subjects following a three-dose schedule at intervals of 28 days. 39 While the safety, reactogenicity and immunogenicity were reported, 40 here we describe additional results which enable to further assess the effect of OMVs on the quality of the antibody response in humans. The analysis was performed with sera from trial participants vaccinated with RBD-d/ OMV/alum (50 mg/20 mg/1250 mg) and RBD-d/alum (50 mg/1250 mg).…”

“…The number of subjects with IgG concentration 470 AU/mL increased after the third dose with respect to the second one: for RBD-d/OMV/alum from 13/20 (65%) to 18/20 (90%) and for RBD-d/alum from 10/20 (50%) to 13/20 (65%). 40 Interestingly, while the IgG response at day 28 after the second (T = 56) and third doses (T = 84) was rather similar, 40 the quality of the IgG response was certainly higher for both formulations on day 28 after the third vaccination (T = 84), as determined by the inhibition of the RBD-ACE2 interaction. In mVNT 50 , the percentage of subjects attaining an ID 50 4 150 comparing the inhibition of the interaction between the phage-displayed RBD mutants and the ACE2 receptor.…”

“…Fig.4Immunogenicity evaluation from a phase I clinical trial 39,40. Subjects immunized with RBD-d/OMV (50 mg/20 mg, blue) vs. RBD-d (50 mg, red) adsorbed in alum.…”

A COVID-19 vaccine candidate composed of the SARS-CoV-2 RBD dimer and Neisseria meningitidis outer membrane vesicles