Protective antibodies and T cell responses to Omicron variant three months after the booster dose of BNT162b2 vaccine

Naaber, Paul; Tserel, Liina; Kangro, Kadri; Sepp, Epp; Jürjenson, Virge; Kärner, Jaanika; Haljasmägi, Liis; Haljasorg, Uku; Kuusk, Marilin; Gerhold, Joachim M.; Planken, Anu; Ustav, Mart; Kisand, Kai; Peterson, Pärt

doi:10.1101/2022.03.04.22271890

Cited by 2 publications

(5 citation statements)

References 30 publications

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“… 71 Overall, this investigation showcases that vaccinated individuals after a second dose were seen to have stronger specific memory T‐cell responses against the SARS‐CoV‐2 virus, and this was further elevated after the third vaccination along with the long time presence of both CD4 + and CD8 + levels with a little lower response towards Omicron variant. 71 …”

Section: T‐cell Immunity Against Sars‐cov‐2 Omicronmentioning

confidence: 62%

“…In another study by Paul Naaber et al, where T‐cell response against Omicron was studied after the booster dose, here participants were vaccinated with two doses of BNT162b2 vaccine and after a gap period of 9 months were vaccinated with a booster dose from BNT162b2, before the booster vaccination the Spike‐RBD immunoglobulin G (IgG) was seen to be in decline after second vaccination but 2 weeks after the booster dose the IgG levels were found to be higher than the previous level, however, 3 months after the booster dose the IgG level was seen to be lower in comparison to its initial levels. In this study, 71 Omicron‐specific CD4 + and CD8 + T‐cell responses and activation‐induced marker (AIM) memory T cells in CD4 + and CD8 + T cells were investigated after the second vaccination and after the third/booster vaccination. Before the administering the third dose the 84% of vaccinated participants were found to have CD4 + memory response and 58% of participants with CD8 + memory response after the booster dose the number was increased to 100% in CD4 + and 90% CD8 + and the Spike‐specific T cells were found to be higher after 2 weeks of booster dose in CD4 + in comparison with CD8 + levels and after 3 months of booster vaccination the Spike specific CD4 + T cells were still present in vaccinees 71 .…”

Section: T‐cell Immunity Against Sars‐cov‐2 Omicronmentioning

confidence: 99%

“…In this study, 71 Omicron‐specific CD4 + and CD8 + T‐cell responses and activation‐induced marker (AIM) memory T cells in CD4 + and CD8 + T cells were investigated after the second vaccination and after the third/booster vaccination. Before the administering the third dose the 84% of vaccinated participants were found to have CD4 + memory response and 58% of participants with CD8 + memory response after the booster dose the number was increased to 100% in CD4 + and 90% CD8 + and the Spike‐specific T cells were found to be higher after 2 weeks of booster dose in CD4 + in comparison with CD8 + levels and after 3 months of booster vaccination the Spike specific CD4 + T cells were still present in vaccinees 71 . Overall, this investigation showcases that vaccinated individuals after a second dose were seen to have stronger specific memory T‐cell responses against the SARS‐CoV‐2 virus, and this was further elevated after the third vaccination along with the long time presence of both CD4 + and CD8 + levels with a little lower response towards Omicron variant 71 …”

Section: T‐cell Immunity Against Sars‐cov‐2 Omicronmentioning

confidence: 99%

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Molecular aspects of Omicron, vaccine development, and recombinant strain XE: A review

Akash

Sharma

Kumar

et al. 2022

Journal of Medical Virology

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The global pandemic of COVID-19 began in December 2019 and is still continuing.The past 2 years have seen the emergence of several variants that were more vicious than each other. The emergence of Omicron (B.1.1.529) proved to be a huge epidemiological concern as the rate of infection of this particular strain was enormous. The strain was identified in South Africa on November 24, 2021 and was classified as a "Variant of Concern" on November 26, 2021. The Omicron variant possessed mutations in the key RBD region, the S region, thereby increasing the affinity of ACE2 for better transmission of the virus. Antibody resistance was found in this variant and it was able to reduce vaccine efficiency of vaccines. The need for a booster vaccine was brought forth due to the prevalence of the Omicron variant and, subsequently, this led to targeted research and development of variant-specific vaccines and booster dosage. This review discusses broadly the genomic characters and features of Omicron along with its specific mutations, evolution, antibody resistance, and evasion, utilization of CRISPR-Cas12a assay for Omicron detection, T-cell immunity elicited by vaccines against Omicron, and strategies to decrease Omicron infection along with COVID-19 and it also discusses on XE recombinant variant and on infectivity of BA.2 subvariant of Omicron.

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Section: T‐cell Immunity Against Sars‐cov‐2 Omicronmentioning

confidence: 62%

Section: T‐cell Immunity Against Sars‐cov‐2 Omicronmentioning

confidence: 99%

Section: T‐cell Immunity Against Sars‐cov‐2 Omicronmentioning

confidence: 99%

See 1 more Smart Citation

Molecular aspects of Omicron, vaccine development, and recombinant strain XE: A review

Akash

Sharma

Kumar

et al. 2022

Journal of Medical Virology

View full text Add to dashboard Cite

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“…Observational studies evaluating the effect of vaccination on previously infected individuals reported that antibody levels peaked after three immune stimuli, either by vaccine or infection, without any significant increment after a fourth stimulus [ 21 , 22 ]. On the other hand, cellular immunity seems to stay robust against the Omicron variant after 3 months [ 23 ]. It plays a significant role in protecting against severe disease [ 24 , 25 ].…”

Section: Discussionmentioning

confidence: 99%

“…It plays a significant role in protecting against severe disease [ 24 , 25 ]. It likely will stay highly effective against variants of the SARS-CoV-2 virus due to the capacity of T cells to still recognize mutated epitopes from SARS-CoV-2 [ 23 , 25 , 26 ]. Consistent with data on cellular immunity, we observed a slight waning of protection against severe outcomes in the Omicron period.…”

Section: Discussionmentioning

confidence: 99%

Effectiveness of mRNA boosters after homologous primary series with BNT162b2 or ChAdOx1 against symptomatic infection and severe COVID-19 in Brazil and Scotland: A test-negative design case–control study

et al. 2023

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Background Brazil and Scotland have used mRNA boosters in their respective populations since September 2021, with Omicron’s emergence accelerating their booster program. Despite this, both countries have reported substantial recent increases in Coronavirus Disease 2019 (COVID-19) cases. The duration of the protection conferred by the booster dose against symptomatic Omicron cases and severe outcomes is unclear. Methods and findings Using a test-negative design, we analyzed national databases to estimate the vaccine effectiveness (VE) of a primary series (with ChAdOx1 or BNT162b2) plus an mRNA vaccine booster (with BNT162b2 or mRNA-1273) against symptomatic Severe Acute Respiratory Syndrome Coronavirus 2 (SARS-CoV-2) infection and severe COVID-19 outcomes (hospitalization or death) during the period of Omicron dominance in Brazil and Scotland compared to unvaccinated individuals. Additional analyses included stratification by age group (18 to 49, 50 to 64, ≥65). All individuals aged 18 years or older who reported acute respiratory illness symptoms and tested for SARS-CoV-2 infection between January 1, 2022, and April 23, 2022, in Brazil and Scotland were eligible for the study. At 14 to 29 days after the mRNA booster, the VE against symptomatic SARS-CoV-2 infection of ChAdOx1 plus BNT162b2 booster was 51.6%, (95% confidence interval (CI): [51.0, 52.2], p < 0.001) in Brazil and 67.1% (95% CI [65.5, 68.5], p < 0.001) in Scotland. At ≥4 months, protection against symptomatic infection waned to 4.2% (95% CI [0.7, 7.6], p = 0.02) in Brazil and 37.4% (95% CI [33.8, 40.9], p < 0.001) in Scotland. VE against severe outcomes in Brazil was 93.5% (95% CI [93.0, 94.0], p < 0.001) at 14 to 29 days post-booster, decreasing to 82.3% (95% CI [79.7, 84.7], p < 0.001) and 98.3% (95% CI [87.3, 99.8], p < 0.001) to 77.8% (95% CI [51.4, 89.9], p < 0.001) in Scotland for the same periods. Similar results were obtained with the primary series of BNT162b2 plus homologous booster. Potential limitations of this study were that we assumed that all cases included in the analysis were due to the Omicron variant based on the period of dominance and the limited follow-up time since the booster dose. Conclusions We observed that mRNA boosters after a primary vaccination course with either mRNA or viral-vector vaccines provided modest, short-lived protection against symptomatic infection with Omicron but substantial and more sustained protection against severe COVID-19 outcomes for at least 3 months.

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Protective antibodies and T cell responses to Omicron variant three months after the booster dose of BNT162b2 vaccine

Cited by 2 publications

References 30 publications

Molecular aspects of Omicron, vaccine development, and recombinant strain XE: A review

Molecular aspects of Omicron, vaccine development, and recombinant strain XE: A review

Effectiveness of mRNA boosters after homologous primary series with BNT162b2 or ChAdOx1 against symptomatic infection and severe COVID-19 in Brazil and Scotland: A test-negative design case–control study

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