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Heterologous COVID-19 vaccine schedule with protein-based prime (NVX-CoV2373) and mRNA boost (BNT162b2) induces strong humoral responses: results from COV-BOOST trial

Heterologous COVID-19 vaccine schedule with protein-based prime (NVX-CoV2373) and mRNA boost (BNT162b2) induces strong humoral responses: results from COV-BOOST trial
Heterologous COVID-19 vaccine schedule with protein-based prime (NVX-CoV2373) and mRNA boost (BNT162b2) induces strong humoral responses: results from COV-BOOST trial
Background: heterologous schedules of booster vaccines for COVID-19 following initial doses of mRNA or adenoviral vector vaccines have been shown to be safe and immunogenic. There are few data on booster doses following initial doses of protein nanoparticle vaccines.

Methods: participants of the phase 3 clinical trial of the COVID-19 vaccine NVX-CoV2373 (EudraCT 2020–004123-16) enroled between September 28 and November 28, 2020, who received 2 doses of NVX-CoV2373 administered 21 days apart were invited to receive a third dose booster vaccine of BNT162b2 (wild type mRNA vaccine) as a sub-study of the COV-BOOST clinical trial, and were followed up for assessment of safety, reactogenicity and immunogenicity to day 242 post-booster.

Results: the BNT162b2 booster following two doses of NVX-COV2373 was well-tolerated. Most adverse events were mild to moderate, with no serious vaccine-related adverse events reported. Immunogenicity analysis showed a significant increase in spike IgG titres and T-cell responses post-third dose booster. Specifically, IgG levels peaked at day 14 with a geometric mean concentration (GMC) of 216,255 ELISA laboratory units (ELU)/mL (95% CI 191,083–244,743). The geometric mean fold increase from baseline to day 28 post-boost was 168.6 (95% CI 117.5–241.8). Spike IgG titres were sustained above baseline levels at day 242 with a GMC of 58,686 ELU/mL (95% CI 48,954–74,652), with significant decay between days 28 and 84 (geometric mean ratio 0.58, 95% CI 0.53–0.63). T-cell responses also demonstrated enhancement post-booster, with a geometric mean fold increase of 5.1 (95% CI 2.9–9.0) at day 14 in fresh samples and 3.0 (95% CI 1.8–4.9) in frozen samples as measured by ELISpot. In an exploratory analysis, participants who received BNT162b2 after two doses of NVX-COV2373 exhibited higher anti-spike IgG at Day 28 than those who received homologous three doses of BNT162b2, with a GMR of 5.02 (95% CI: 3.17–7.94). This trend remained consistent across all time points, indicating a similar decay rate between the two schedules.

Conclusions: a BNT162b2 third dose booster dose in individuals primed with two doses of NVX-COV2373 is safe and induces strong and durable immunogenic responses, higher than seen in other comparable studies. These findings support the use and investigation of heterologous booster strategies and early investigation of heterologous vaccine technology schedules should be a priority in the development of vaccines against new pathogens.
BNT162b2, Booster, COVID-19, NVX-CoV2373, Novavax, Pfizer, SARS-CoV-2, Vaccine
0163-4453
Janani, Leila
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Munro, Alasdair P.S.
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Wright, Annie
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Aley, Parvinder K.
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Baxter, David
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Bawa, Tanveer
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Bibi, Sagida
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Bula, Marcin
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Cathie, Katrina
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Chatterjee, Krishna
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Enever, Yvanne
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Galiza, Eva
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Harris, Mae
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Hicks, Alexander
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Jones, Christine E.
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Kanji, Nasir
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van der Klaauw, Agatha A.
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Libri, Vincenzo
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Llewelyn, Martin J.
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Mansfield, Rebecca
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McGregor, Alastair C.
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Minassian, Angela M.
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Moore, Patrick
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Mujadidi, Yama F.
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Belhadef, Hanane Trari
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Holliday, Kyra
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Osanlou, Orod
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Osanlou, Rostam
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Pacurar, Mihaela
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Palfreeman, Adrian
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Regan, Karen
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Saich, Stephen
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Saralaya, Dinesh
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Sharma, Sunil
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Sheridan, Ray
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Stokes, Matthew
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Thomson, Emma C.
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Todd, Shirley
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Twelves, Chris
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Wright, Daniel
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Read, Robert C.
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Charlton, Sue
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Hallis, Bassam
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Ramsay, Mary
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Andrews, Nick
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Faust, Saul N.
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COV-BOOST study group
Janani, Leila
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Munro, Alasdair P.S.
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Wright, Annie
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Aley, Parvinder K.
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Babbage, Gavin
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Baxter, David
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Bawa, Tanveer
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Bibi, Sagida
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Bula, Marcin
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Cathie, Katrina
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Chatterjee, Krishna
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Cosgrove, Catherine
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Enever, Yvanne
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Galiza, Eva
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Goodman, Anna L.
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Green, Christopher A.
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Harris, Mae
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Hicks, Alexander
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Jones, Christine E.
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Kanji, Nasir
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van der Klaauw, Agatha A.
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Libri, Vincenzo
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Llewelyn, Martin J.
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Mansfield, Rebecca
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McGregor, Alastair C.
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Minassian, Angela M.
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Moore, Patrick
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Mujadidi, Yama F.
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Belhadef, Hanane Trari
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Holliday, Kyra
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Osanlou, Orod
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Osanlou, Rostam
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Pacurar, Mihaela
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Palfreeman, Adrian
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Regan, Karen
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Saich, Stephen
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Saralaya, Dinesh
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Sharma, Sunil
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Sheridan, Ray
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Stokes, Matthew
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Thomson, Emma C.
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Todd, Shirley
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Twelves, Chris
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Wright, Daniel
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Read, Robert C.
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Charlton, Sue
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Hallis, Bassam
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Ramsay, Mary
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Andrews, Nick
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Faust, Saul N.
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Janani, Leila, Munro, Alasdair P.S. and Wright, Annie , COV-BOOST study group (2025) Heterologous COVID-19 vaccine schedule with protein-based prime (NVX-CoV2373) and mRNA boost (BNT162b2) induces strong humoral responses: results from COV-BOOST trial. Journal of Infection, 91 (3), [106576]. (doi:10.1016/j.jinf.2025.106576).

Record type: Article

Abstract

Background: heterologous schedules of booster vaccines for COVID-19 following initial doses of mRNA or adenoviral vector vaccines have been shown to be safe and immunogenic. There are few data on booster doses following initial doses of protein nanoparticle vaccines.

Methods: participants of the phase 3 clinical trial of the COVID-19 vaccine NVX-CoV2373 (EudraCT 2020–004123-16) enroled between September 28 and November 28, 2020, who received 2 doses of NVX-CoV2373 administered 21 days apart were invited to receive a third dose booster vaccine of BNT162b2 (wild type mRNA vaccine) as a sub-study of the COV-BOOST clinical trial, and were followed up for assessment of safety, reactogenicity and immunogenicity to day 242 post-booster.

Results: the BNT162b2 booster following two doses of NVX-COV2373 was well-tolerated. Most adverse events were mild to moderate, with no serious vaccine-related adverse events reported. Immunogenicity analysis showed a significant increase in spike IgG titres and T-cell responses post-third dose booster. Specifically, IgG levels peaked at day 14 with a geometric mean concentration (GMC) of 216,255 ELISA laboratory units (ELU)/mL (95% CI 191,083–244,743). The geometric mean fold increase from baseline to day 28 post-boost was 168.6 (95% CI 117.5–241.8). Spike IgG titres were sustained above baseline levels at day 242 with a GMC of 58,686 ELU/mL (95% CI 48,954–74,652), with significant decay between days 28 and 84 (geometric mean ratio 0.58, 95% CI 0.53–0.63). T-cell responses also demonstrated enhancement post-booster, with a geometric mean fold increase of 5.1 (95% CI 2.9–9.0) at day 14 in fresh samples and 3.0 (95% CI 1.8–4.9) in frozen samples as measured by ELISpot. In an exploratory analysis, participants who received BNT162b2 after two doses of NVX-COV2373 exhibited higher anti-spike IgG at Day 28 than those who received homologous three doses of BNT162b2, with a GMR of 5.02 (95% CI: 3.17–7.94). This trend remained consistent across all time points, indicating a similar decay rate between the two schedules.

Conclusions: a BNT162b2 third dose booster dose in individuals primed with two doses of NVX-COV2373 is safe and induces strong and durable immunogenic responses, higher than seen in other comparable studies. These findings support the use and investigation of heterologous booster strategies and early investigation of heterologous vaccine technology schedules should be a priority in the development of vaccines against new pathogens.

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e-pub ahead of print date: 7 August 2025
Published date: September 2025
Keywords: BNT162b2, Booster, COVID-19, NVX-CoV2373, Novavax, Pfizer, SARS-CoV-2, Vaccine

Identifiers

Local EPrints ID: 505644
URI: http://eprints.soton.ac.uk/id/eprint/505644
ISSN: 0163-4453
PURE UUID: f8e8fd76-62a0-4582-a298-d93a217e7cf4
ORCID for Katrina Cathie: ORCID iD orcid.org/0000-0001-5074-0769
ORCID for Christine E. Jones: ORCID iD orcid.org/0000-0003-1523-2368
ORCID for Robert C. Read: ORCID iD orcid.org/0000-0002-4297-6728
ORCID for Saul N. Faust: ORCID iD orcid.org/0000-0003-3410-7642

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Date deposited: 15 Oct 2025 16:39
Last modified: 16 Oct 2025 01:52

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Contributors

Author: Leila Janani
Author: Alasdair P.S. Munro
Author: Annie Wright
Author: Parvinder K. Aley
Author: Gavin Babbage
Author: David Baxter
Author: Tanveer Bawa
Author: Sagida Bibi
Author: Marcin Bula
Author: Katrina Cathie ORCID iD
Author: Krishna Chatterjee
Author: Catherine Cosgrove
Author: Yvanne Enever
Author: Eva Galiza
Author: Anna L. Goodman
Author: Christopher A. Green
Author: Mae Harris
Author: Alexander Hicks
Author: Nasir Kanji
Author: Agatha A. van der Klaauw
Author: Vincenzo Libri
Author: Martin J. Llewelyn
Author: Rebecca Mansfield
Author: Alastair C. McGregor
Author: Angela M. Minassian
Author: Patrick Moore
Author: Yama F. Mujadidi
Author: Hanane Trari Belhadef
Author: Kyra Holliday
Author: Orod Osanlou
Author: Rostam Osanlou
Author: Mihaela Pacurar
Author: Adrian Palfreeman
Author: Karen Regan
Author: Stephen Saich
Author: Dinesh Saralaya
Author: Sunil Sharma
Author: Ray Sheridan
Author: Matthew Stokes
Author: Emma C. Thomson
Author: Shirley Todd
Author: Chris Twelves
Author: Daniel Wright
Author: Robert C. Read ORCID iD
Author: Sue Charlton
Author: Bassam Hallis
Author: Mary Ramsay
Author: Nick Andrews
Author: Saul N. Faust ORCID iD
Corporate Author: COV-BOOST study group

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