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Immunogenicity of a fractional or full third dose of AZD1222 vaccine or BNT162b2 messenger RNA vaccine after two doses of CoronaVac vaccines against the Delta and Omicron variants
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Document Title
Immunogenicity of a fractional or full third dose of AZD1222 vaccine or BNT162b2 messenger RNA vaccine after two doses of CoronaVac vaccines against the Delta and Omicron variants
Author
Niyomnaitham S. Jongkaewwattana A. Meesing A. Pinpathomrat N. Nanthapisal S. Hirankarn N. Siwamogsatham S. Kirdlarp S. Chaiwarith R. Lawpoolsri S. Phanthanawiboon S. Thitithanyanont A. Hansasuta P. Chaiyaroj S. Pitisuttithum P.
Affiliations
Department of Pharmacology Faculty of Medicine Siriraj Hospital Mahidol University Bangkok Thailand; National Center for Genetic Engineering and Biotechnology National Science and Technology Development Agency Pathumthani Thailand; Division of Infectious Diseases and Tropical Medicine Department of Medicine Faculty of Medicine Khon Kaen University Khon Kaen Thailand; Clinical Research Center Faculty of Medicine Prince of Songkla University Songkhla Thailand; Clinical Research Center Faculty of Medicine Thammasat University Pathumthani Thailand; Department of Microbiology Faculty of Medicine Chulalongkorn University Bangkok Thailand; Maha Chakri Sirindhorn Clinical Research Center Faculty of Medicine Chulalongkorn University Bangkok Thailand; Chakri Naruebodindra Medical Institute Faculty of Medicine Ramathibodi Hospital Mahidol University Samut Prakarn Thailand; Division of Infectious Diseases and Tropical Medicine Department of Internal Medicine Faculty of Medicine Chiang Mai University Chiang Mai Thailand; Faculty of Tropical Medicine Mahidol University Bangkok Thailand; Department of Microbiology Faculty of Medicine Khon Kaen University Khon Kaen Thailand; Faculty of Science Mahidol University Bangkok Thailand; Division of Virology Department of Microbiology Faculty of Medicine Chulalongkorn University Bangkok Thailand; Department of Microbiology Faculty of Science Mahidol University Bangkok Thailand; Vaccine Trial Centre Faculty of Tropical Medicine Mahidol University Bangkok Thailand
Type
Article
Source Title
International Journal of Infectious Diseases
ISSN
12019712
Year
2023
Volume
129
Page
19-31
Open Access
All Open Access Gold Green
Publisher
Elsevier B.V.
DOI
10.1016/j.ijid.2023.01.022
Abstract
Objectives: The study aimed to compare the immunogenicity and safety of fractional (half) third doses of heterologous COVID-19 vaccines (AZD1222 or BNT162b2) to full doses after the two-dose CoronaVac and when boosting after three different extended intervals. Methods: At 60-<90 90-<120 or 120-180 days intervals after the two-dose CoronaVac participants were randomized to full-dose or half-dose AZD1222 or BNT162b2 followed up at day 28 60 and 90. Vaccination-induced immune responses to Ancestral Delta and Omicron BA.1 strains were evaluated by antispike pseudovirus and microneutralization and T cell assays. Descriptive statistics and noninferiority cut-offs were reported as geometric mean concentration or titer and concentration or titer ratios comparing baseline to day 28 and day 90 and different intervals. Results: No safety concerns were detected. All assays and intervals showed noninferior immunogenicity between full doses and half doses. However full-dose vaccines and/or longer 120-180-day intervals substantially improved the immunogenicity (measured by antispike or measured by pseudotyped virus neutralizing titers 50; P <0.001). Seroconversion rates were over 90% against the SARS-CoV-2 strains by all assays. Immunogenicity waned more quickly with half doses than full doses but remained high against the Ancestral or Delta strains. Against Omicron the day 28 immunogenicity increased with longer intervals than shorter intervals for full-dose vaccines. Conclusion: Immune responses after day 28 when boosting at longer intervals after the two-dose CoronaVac was optimal. Half doses met the noninferiority criteria compared with the full dose by all the immune assays assessed. ? 2023 The Author(s)
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License
CC BY
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Publication Source
WOS