Single-cell BCR and transcriptome analysis after influenza infection reveals spatiotemporal dynamics of antigen-specific B cells
Abstract
B cell responses are critical for antiviral immunity. However, a comprehensive picture of antigen-specific B cell differentiation, clonal proliferation, and dynamics in different organs after infection is lacking. Here, by combining single-cell RNA and B cell receptor (BCR) sequencing of antigen-specific cells in lymph nodes, spleen, and lungs after influenza infection in mice, we identify several germinal center (GC) B cell subpopulations and organ-specific differences that persist over the course of the response. We discover transcriptional differences between memory cells in lungs and lymphoid organs and organ-restricted clonal expansion. Remarkably, we find significant clonal overlap between GC-derived memory and plasma cells. By combining BCR-mutational analyses with monoclonal antibody (mAb) expression and affinity measurements, we find that memory B cells are highly diverse and can be selected from both low- and high-affinity precursors. By linking antigen recognition with transcriptional programming, clonal proliferation, and differentiation, these finding provide important advances in our understanding of antiviral immunity.
Citation
Cell reports, 35 (12), 109286
Collections
View/ Open
Date
2022Author
Mathew, Nimitha Rose
Jayanthan, Jayalal
Smirnov, Ilya
Robinson, Jonathan L
Axelsson, Hannes
Sowdamini Nakka, Sravya
Emmanouilidi, Aikaterini
Czarnewski, Paulo
Yewdell, William T
Schön, Karin
Lebrero-Fernandez, Cristina
Bernasconi, Valentina
Rodin, William
Harandi, Ali M
Lycke, Nils Y
Borcherding, Nicholas
Yewdell, Jonathan W
Greiff, Victor
Bemark, Mats
Angeletti, Davide
Publication type
article, peer reviewed scientific
Language
eng