Persistence of immunity and impact of third dose of inactivated COVID-19 vaccine against emerging variants

Krishna Mohan Vadrevu, Brunda Ganneru, Siddharth Reddy, Harsh Jogdand, Dugyala Raju, Gajanan Sapkal, Pragya Yadav, Prabhakar Reddy, Savita Verma, Chandramani Singh, Sagar Vivek Redkar, Chandra Sekhar Gillurkar, Jitendra Singh Kushwaha, Satyajit Mohapatra, Amit Bhate, Sanjay Kumar Rai, Raches Ella, Priya Abraham, Sai Prasad, Krishna Ella, Krishna Mohan Vadrevu, Brunda Ganneru, Siddharth Reddy, Harsh Jogdand, Dugyala Raju, Gajanan Sapkal, Pragya Yadav, Prabhakar Reddy, Savita Verma, Chandramani Singh, Sagar Vivek Redkar, Chandra Sekhar Gillurkar, Jitendra Singh Kushwaha, Satyajit Mohapatra, Amit Bhate, Sanjay Kumar Rai, Raches Ella, Priya Abraham, Sai Prasad, Krishna Ella

Abstract

This is a comprehensive report on immunogenicity of COVAXIN® booster dose against ancestral and Variants of Concern (VOCs) up to 12 months. It is well known that neutralizing antibodies induced by COVID-19 vaccines wane within 6 months of vaccination leading to questions on the effectiveness of two-dose vaccination against breakthrough infections. Therefore, we assessed the persistence of immunogenicity up to 6 months after a two or three-dose with BBV152 and the safety of a booster dose in an ongoing phase 2, double-blind, randomized controlled trial (ClinicalTrials.gov: NCT04471519). We report persistence of humoral and cell mediated immunity up to 12 months of vaccination, despite decline in the magnitude of antibody titers. Administration of a third dose of BBV152 increased neutralization titers against both homologous (D614G) and heterologous strains (Alpha, Beta, Delta, Delta Plus and Omicron) with a slight increase in B cell memory responses. Thus, seronversion rate remain high in boosted recipients compared to non-booster, even after 6 months, post third dose against variants. No serious adverse events observed, except pain at the injection site, itching and redness. Hence, these results indicate that a booster dose of BBV152 is safe and necessary to ensure persistent immunity to minimize breakthrough infections of COVID-19, due to newly emerging variants.Trial registration: Registered with the Clinical Trials Registry (India) No. CTRI/2021/04/032942, dated 19/04/2021 and on Clinicaltrials.gov: NCT04471519.

Conflict of interest statement

The authors declare no competing interests.

© 2022. The Author(s).

Figures

Figure 1
Figure 1
Study flow chart.
Figure 2
Figure 2
Persistence of T and B cell memory responses against SARS-CoV-2 (D614G). Boxes display the SARS-CoV-2-specific T and B cell memory responsesafter two doses of BBV152 on Days 0 and 28 measured on Day 215 (before booster dose) and Day 243 (28 days after the booster dose of BBV152). PBMC samples collected from 15 participants (n = 8 non-booster and n = 7 BBV152 recipients). Boxes indicate upper and lower quartiles,lines within the box indicate median and whiskers extending from the boxes indicate the upper and lower quartiles.*p 

Figure 3

Vaccine-induced antigen-specific antibody (IgG and…

Figure 3

Vaccine-induced antigen-specific antibody (IgG and IgA) secreting memory B-cell responses performed by ELISpot…

Figure 3
Vaccine-induced antigen-specific antibody (IgG and IgA) secreting memory B-cell responses performed by ELISpot assay. PBMCs collected from vaccinated subjects on Day 215 were pre-activated or pre-stimulated with polyclonal expansion using Poly B stimulant for 4 days, with unstimulated cells or cells without pre-activation as negative controls. Antibody-secreting cells (ASC) were detected with anti-human IgG (biotin) and anti-human IgA (FITC) antibody followed by streptavidin–ALP and FITC-HRP respectively. Boxes indicate upper and lower quartiles, lines within the box indicate median and whiskers extending from the boxes indicate the upper and lower quartiles.

Figure 4

Persistence of SARS-CoV-2 antigen recall…

Figure 4

Persistence of SARS-CoV-2 antigen recall T cell responses until 12 months post 2nd…

Figure 4
Persistence of SARS-CoV-2 antigen recall T cell responses until 12 months post 2nd dose and increased memory B cell response with the booster dose. PBMCs collected on Day 395 were used for both the assays.
Figure 3
Figure 3
Vaccine-induced antigen-specific antibody (IgG and IgA) secreting memory B-cell responses performed by ELISpot assay. PBMCs collected from vaccinated subjects on Day 215 were pre-activated or pre-stimulated with polyclonal expansion using Poly B stimulant for 4 days, with unstimulated cells or cells without pre-activation as negative controls. Antibody-secreting cells (ASC) were detected with anti-human IgG (biotin) and anti-human IgA (FITC) antibody followed by streptavidin–ALP and FITC-HRP respectively. Boxes indicate upper and lower quartiles, lines within the box indicate median and whiskers extending from the boxes indicate the upper and lower quartiles.
Figure 4
Figure 4
Persistence of SARS-CoV-2 antigen recall T cell responses until 12 months post 2nd dose and increased memory B cell response with the booster dose. PBMCs collected on Day 395 were used for both the assays.

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