Multimodal characterization of antigen-specific CD8+T cells across SARS-CoV-2 vaccination and infection

Author:

Zhang BingjieORCID,Upadhyay RabiORCID,Hao YuhanORCID,Samanovic Marie I.ORCID,Herati Ramin S.ORCID,Blair JohnORCID,Axelrad JordanORCID,Mulligan Mark J.ORCID,Littman Dan R.ORCID,Satija RahulORCID

Abstract

ABSTRACTThe human 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 utilize multimodal sequencing technologies to perform a longitudinal analysis of circulating human leukocytes collected before and after BNT162b2 immunization. Our data reveal distinct subpopulations of CD8+T cells which reliably appear 28 days after prime vaccination (7 days post boost). Using a suite of cross-modality integration tools, we define their transcriptome, accessible chromatin landscape, and immunophenotype, and identify unique biomarkers within each modality. By leveraging DNA-oligo-tagged peptide-MHC multimers and T cell receptor sequencing, we demonstrate that this vaccine-induced population is SARS-CoV-2 antigen-specific and capable of rapid clonal expansion. Moreover, we also identify these CD8+populations in scRNA-seq datasets from COVID-19 patients and find that their relative frequency and differentiation outcomes are predictive of subsequent clinical outcomes. Our work contributes to our understanding of T cell immunity, and highlights the potential for integrative and multimodal analysis to characterize rare cell populations.

Publisher

Cold Spring Harbor Laboratory

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