Safety, reactogenicity, and immunogenicity of homologous and heterologous prime-boost immunisation with ChAdOx1-nCoV19 and BNT162b2: a prospective cohort study

Hillus, David, Schwarz, Tatjana, Tober-Lau, Pinkus, Hastor, Hana, Thibeault, Charlotte, Kasper, Stefanie, Helbig, Elisa, Lippert, Lena, Tscheak, Patricia, Schmidt, Marie Luisa, Riege, Johanna, Solarek, André, Kalle, Christof von, Dang-Heine, Chantip, Kopankiewicz, Piotr, Suttorp, Norbert, Drosten, Christian, Bias, Harald, Seybold, Joachim, Conrad, Claudia, Steuer, Doris, Gläser, Ute, Sinnigen, Anne-Sophie, Rubisch, Carolin, Olk, Nadine, Hasler, Lisbeth, Sanchez-Rezza, Angela, Kronenberg, Paolo, Horn, Alexandra, Koch, Willi, Stubbemann, Paula, Gabelich, Julie-Anne, Münn, Friederike, Tesch, Julia, Mackeldanz, Petra, Bergfeld, Leon, Bleicker, Tobias, Beheim-Schwarzbach, Jörn Ilmo, Hiller, Anna, Brumhard, Sophia, Bardtke, Lara, Pohl, Kai, Wendisch, Daniel, Georg, Philipp, Treue, Denise, Briesemeister, Dana, Schlesinger, Jenny, Hetey, Andreas, Kegel, Luisa, Richter, Annelie, Al-Rim, Ben, Maeß, Birgit, Behn, Kerstin, Lysi, Michelle, Zvorc, Saskia, Rönnefarth, Maria, Schmidt, Sein, Krannich, Alexander, Schellenberger, Isabelle, Schwanitz, Georg, Schenkel, Viktoria, Bethke, Norma, Hülso, Claudia, Dieckmann, Sebastian, Peiser, Christian, Kurth, Florian, Corman, Victor Max, Sander, Leif Erik, Group, Eicov Covim Study

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Safety, reactogenicity, and immunogenicity of homologous and heterologous prime-boost immunisation with ChAdOx1-nCoV19 and BNT162b2: a prospective cohort study

Hillus, David, Schwarz, Tatjana, Tober-Lau, Pinkus, Hastor, Hana, Thibeault, Charlotte, Kasper, Stefanie, Helbig, Elisa, Lippert, Lena, Tscheak, Patricia, Schmidt, Marie Luisa, Riege, Johanna, Solarek, André, Kalle, Christof von, Dang-Heine, Chantip, Kopankiewicz, Piotr, Suttorp, Norbert, Drosten, Christian, Bias, Harald, Seybold, Joachim, Conrad, Claudia, Steuer, Doris, Gläser, Ute, Sinnigen, Anne-Sophie, Rubisch, Carolin, Olk, Nadine, Hasler, Lisbeth, Sanchez-Rezza, Angela, Kronenberg, Paolo, Horn, Alexandra, Koch, Willi, Stubbemann, Paula, Gabelich, Julie-Anne, Münn, Friederike, Tesch, Julia, Mackeldanz, Petra, Bergfeld, Leon, Bleicker, Tobias, Beheim-Schwarzbach, Jörn Ilmo, Hiller, Anna, Brumhard, Sophia, Bardtke, Lara, Pohl, Kai, Wendisch, Daniel, Georg, Philipp, Treue, Denise, Briesemeister, Dana, Schlesinger, Jenny, Hetey, Andreas, Kegel, Luisa, Richter, Annelie, Al-Rim, Ben, Maeß, Birgit, Behn, Kerstin, Lysi, Michelle, Zvorc, Saskia, Rönnefarth, Maria, Schmidt, Sein, Krannich, Alexander, Schellenberger, Isabelle, Schwanitz, Georg, Schenkel, Viktoria, Bethke, Norma, Hülso, Claudia, Dieckmann, Sebastian, Peiser, Christian, Kurth, Florian, Corman, Victor Max, Sander, Leif Erik, Group, Eicov Covim Study.

2021.

Preprint in English | Other preprints | ID: ppcovidwho-294933

ABSTRACT

ABSTRACT

Objective to assess reactogenicity and immunogenicity of heterologous prime-boost immunisations of ChAdOx1-nCoV19 (Vaxzevria, ChAdOx) followed by BNT162b2 (Comirnaty, BNT) compared to homologous BNT/BNT immunisation. Design prospective, observational cohort study. Setting unicenter study in a cohort of health care workers at a tertiary care center in Berlin, Germany. Participants 340 health care workers immunised between 27 December 2020 and 21 May 2021 at Charité - Universitätsmedizin Berlin, Germany Main outcome measures the main outcomes were reactogenicity assessed on days one, three, five and seven post prime and boost vaccination, and immunogenicity measured by serum SARS-CoV-2 full spike-, spike S1-, and spike RBD-IgG, virus neutralisation capacity, anti-S1-IgG avidity, and T cell reactivity measured by Interferon gamma release assay at 3-4 weeks post prime and boost immunisation. Results Heterologous ChAdOx/BNT booster vaccination was overall well-tolerated and reactogenicity was largely comparable to homologous BNT/BNT vaccination. Systemic reactions were most frequent after prime immunisation with ChAdOx (86%, 95CI 79-91), and less frequent after homologous BNT/BNT (65%, 95CI 56-72), or heterologous ChAdOx/BNT booster vaccination (48%, 95CI 36-59). Serum antibody responses and T cell reactivity were strongly increased after both homologous and heterologous boost, and immunogenicity was overall robust, and comparable between both regimens in this cohort, with slightly increased S1-IgG avidity and T cell responses following heterologous booster immunisation. Conclusions Evidence of rare thrombotic events associated with ChAdOx has led to recommendation of a heterologous booster with mRNA vaccines for certain age groups in several European countries, despite a lack of robust safety and immunogenicity data for this vaccine regimen. This interim analysis provides evidence that the currently recommended heterologous ChAdOx/BNT immunisation regimen with 10-12 week vaccine intervals is well tolerated and slightly more immunogenic compared to homologous BNT/BNT vaccination with three week vaccine intervals. Heterologous prime-boost immunisation for COVID-19 may be generally applicable to optimise logistics and improve immunogenicity and to mitigate potential intermittent supply shortages for individual vaccines.

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Full text: Available Collection: Preprints Database: Other preprints Language: English Year: 2021 Document Type: Preprint

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Full text: Available Collection: Preprints Database: Other preprints Language: English Year: 2021 Document Type: Preprint