Publication date: Sep 21, 2023
The immune response to SARS-CoV-2 antigen after infection or vaccination is defined by the durable production of antibodies and T cells. Population-based monitoring typically focuses on antibody titer, but there is a need for improved characterization and quantification of T cell responses. Here, we used multimodal sequencing technologies to perform a longitudinal analysis of circulating human leukocytes collected before and after immunization with the mRNA vaccine BNT162b2. Our data indicated distinct subpopulations of CD8 T cells, which reliably appeared 28 days after prime vaccination. Using a suite of cross-modality integration tools, we defined their transcriptome, accessible chromatin landscape and immunophenotype, and we identified unique biomarkers within each modality. We further showed that this vaccine-induced population was SARS-CoV-2 antigen-specific and capable of rapid clonal expansion. Moreover, we identified these CD8 T cell populations in scRNA-seq datasets from COVID-19 patients and found that their relative frequency and differentiation outcomes were predictive of subsequent clinical outcomes.
| Concepts | Keywords |
|---|---|
| Antibodies | Antigen |
| Bnt162b2 | Cd8 |
| Covid | Cells |
| Tools | Cov |
| Vaccination | Defined |
| Identified | |
| Infection | |
| Modality | |
| Multimodal | |
| Outcomes | |
| Population | |
| Sars | |
| Specific | |
| Vaccination | |
| Vaccine |
Semantics
| Type | Source | Name |
|---|---|---|
| disease | IDO | cell |
| disease | VO | vaccination |
| disease | MESH | infection |
| disease | IDO | immune response |
| disease | IDO | production |
| disease | VO | population |
| disease | VO | antibody titer |
| disease | VO | immunization |
| disease | VO | vaccine |
| disease | MESH | COVID-19 |
| disease | VO | frequency |