A systems immunology study comparing innate and adaptive immune responses in adults to COVID-19 mRNA (BNT162b2/mRNA-1273) and adenovirus vectored vaccines (ChAdOx1-S) after the first, second and third doses

Author:

Ryan Feargal J.ORCID,Norton Todd S.,McCafferty Conor,Blake Stephen J.,Stevens Natalie E.ORCID,James Jane,Eden Georgina L.,Tee Yee C.,Benson Saoirse C.ORCID,Masavuli Makutiro G.ORCID,Yeow Arthur ELORCID,Abayasingam ArunasingamORCID,Agapiou DavidORCID,Stevens Hannah,Zecha Jana,Messina Nicole L.,Curtis Nigel,Ignjatovic Vera,Monagle Paul,Tran Huyen,McFadyen James D.,Bull Rowena A.,Grubor-Bauk Branka,Lynn Miriam A.ORCID,Botten Rochelle,Barry Simone E.,Lynn David J.

Abstract

AbstractWe longitudinally profiled immune responses in 102 adults who received BNT162b2 (Pfizer-BioNTech) or ChAdOx1-S (Oxford-AstraZeneca) as their primary vaccinations. Bloods were collected pre-vaccination, 1-7 days after the 1st, 2ndand 3rddoses (BNT162b2 or mRNA-1273) to assess innate and early adaptive responses, and ∼28 days after the 2ndand 3rddoses to assess immunogenicity. Using a multi-omics approach including RNAseq, cytokine multiplex assay, proteomics, lipidomics, and flow cytometry we identified key differences in the immune responses induced by the ChAdOx1-S and BNT162b2 vaccines that were correlated with subsequent antigen-specific antibody and T cell responses or vaccine reactogenicity. We observed that vaccination with ChAdOx1-S but not BNT162b2 induced a memory-like response after the first dose, which was correlated with the expression of several proteins involved in complement and coagulation. The COVID-19 Vaccine Immune Responses Study (COVIRS) thus represents a major resource to understand the immunogenicity and reactogenicity of these COVID-19 vaccines.

Publisher

Cold Spring Harbor Laboratory

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