A third vaccination with a single T cell epitope confers protection in a murine model of SARS-CoV-2 infection.
Iris N PardieckTetje Cornelia van der SluisEsmé T I van der GrachtDominique M B VeerkampFelix M BehrSuzanne van DuikerenGuillaume BeyrendJasper RipReza NadafiElham Beyranvand NejadNils MüllingDena J BrasemMarcel G M CampsSebenzile K MyeniPeter J BredenbeekMarjolein KikkertYeonsu KimLuka Čičin ŠainTamim AbdelaalKlaas P J M van GisbergenKees L M C FrankenJan Wouter DrijfhoutCornelis J M MeliefGerben C M ZondagFerry OssendorpRamon ArensPublished in: Nature communications (2022)
Understanding the mechanisms and impact of booster vaccinations are essential in the design and delivery of vaccination programs. Here we show that a three dose regimen of a synthetic peptide vaccine elicits an accruing CD8 + T cell response against one SARS-CoV-2 Spike epitope. We see protection against lethal SARS-CoV-2 infection in the K18-hACE2 transgenic mouse model in the absence of neutralizing antibodies, but two dose approaches are insufficient to confer protection. The third vaccine dose of the single T cell epitope peptide results in superior generation of effector-memory T cells and tissue-resident memory T cells, and these tertiary vaccine-specific CD8 + T cells are characterized by enhanced polyfunctional cytokine production. Moreover, fate mapping shows that a substantial fraction of the tertiary CD8 + effector-memory T cells develop from re-migrated tissue-resident memory T cells. Thus, repeated booster vaccinations quantitatively and qualitatively improve the CD8 + T cell response leading to protection against otherwise lethal SARS-CoV-2 infection.