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Reactogenicity, Safety, and Serological and Cellular Immunogenicity of a Booster Dose of SARS-CoV-2 mRNA Prototype, Variant, and Bivalent Vaccines (preprint)

Evan J. Anderson; Lisa A. Jackson; Nadine G. Rouphael; Alicia T. Widge; David Montefiori; Nicole A. Doria-Rose; Mehul Suthar; Kristen W. Cohen; Sarah O’Connell; Mat Makowski; Mamodikoe Makhene; Wendy Buchanan; Paul Spearman; C. Buddy Creech; Sijy O’Dell; Stephen D Schmidt; Brett Leav; Hamilton Bennett; Rolando Pajon; Christine M. Posavad; John Hural; John H. Beigel; Jim Albert; Kuleni Abebe; Amanda Eaton; Christina A. Rostad; Paulina A. Rebolledo; Satoshi Kamidani; Daniel S. Graciaa; Rhea Coler; Adrian McDermott; Julie E. Ledgerwood; John R. Mascola; Stephen C. De Rosa; Kathleen M. Neuzil; M. Juliana McElrath; Paul C. Roberts.

researchsquare; 2022.

Preprint in English | PREPRINT-RESEARCHSQUARE | ID: ppzbmed-10.21203.rs.3.rs-1594631.v1

ABSTRACT

Waning immunity after two SARS-CoV-2 mRNA vaccinations and the emergence of variants precipitated the need for booster doses. We evaluated safety and serological and cellular immunogenicity through 6 months after a third mRNA vaccination in adults who received the mRNA-1273 primary series in the Phase 1 trial approximately 9 to 10 months earlier. The booster vaccine formulations included 100 mcg of mRNA-1273, 50 mcg of mRNA-1273.351 that encodes Beta variant spike protein, and bivalent vaccine of 25 mcg each of mRNA-1273 and mRNA-1273.351. A third dose of mRNA vaccine appeared safe with acceptable reactogenicity. Vaccination induced rapid increases in binding and neutralizing antibody titers to D614G, Beta, Delta and Omicron variants that persisted through 6 months post-boost, particularly after administration of Beta-containing vaccines. Spike-specific CD4 + and CD8 + T cells increased to levels similar to those following the second dose. Boost vaccination induced broad and durable humoral and T cell responses. ClinicalTrials.gov numbers NCT04283461 (mRNA-1273 Phase 1) and NCT04785144 (mRNA-1273.351 Phase 1)

Safety and Immunogenicity of a Third Dose of SARS-CoV-2 mRNA Vaccine — An Interim Analysis (preprint)

Evan Anderson; Lisa Jackson; Nadine Rouphael; Alicia Widge; David Montefiori; Nicole Doria-Rose; Mehul Suthar; Kristen Cohen; Sarah O'Connell; Mat Makowski; Mamodikoe Makhene; Wendy Buchanan; Paul Spearman; C. Buddy Creech; Sijy O'Dell; Stephen Schmidt; Brett Leav; Hamilton Bennett; Rolando Pajon; Christine Posavad; John Hural; John Beigel; Jim Albert; Kuleni Abebe; Amanda Eaton; Christina Rostad; Paulina Rebolledo; Satoshi Kamidani; Daniel Graciaa; Rhea Coler; Adrian McDermott; Julie Ledgerwood; John Mascola; Stephen DeRosa; Kathleen Neuzil; M. Juliana McElrath; Paul Roberts.

researchsquare; 2022.

Preprint in English | PREPRINT-RESEARCHSQUARE | ID: ppzbmed-10.21203.rs.3.rs-1222037.v1

ABSTRACT

Waning immunity after two SARS-CoV-2 mRNA vaccinations and the emergence of variants precipitated the need for a third dose of vaccine. We evaluated early safety and immunogenicity after a third mRNA vaccination in adults who received the mRNA-1273 primary series in the Phase 1 trial approximately 9 to 10 months earlier. The booster vaccine formulations included 100 mcg of mRNA-1273, 50 mcg of mRNA-1273.351 that encodes Beta variant spike protein, and bivalent vaccine of 25 mcg each of mRNA-1273 and mRNA-1273.351. A third dose of mRNA vaccine appeared safe with acceptable reactogenicity. Vaccination induced rapid increases in binding and neutralizing antibody titers to D614G, Beta, and Delta variants that were similar or greater than peak responses after the second dose. Spike-specific CD4+ and CD8+ T cells increased to similar levels as after the second dose. A third mRNA vaccination was well tolerated and generated robust humoral and T cell responses. ClinicalTrials.gov numbers NCT04283461 (mRNA-1273 Phase 1) and NCT04785144 (mRNA-1273.351 Phase 1)

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