| Literature DB >> 36065187 |
Helena Todorov1,2, Margaux Prieux3,4, Daphne Laubreton3, Matteo Bouvier4,5, Shaoying Wang3, Simon de Bernard6, Christophe Arpin3, Robrecht Cannoodt1,2,7, Wouter Saelens1,2, Arnaud Bonnaffoux5, Olivier Gandrillon4,8, Fabien Crauste9, Yvan Saeys1,2, Jacqueline Marvel3.
Abstract
In this work, we studied the generation of memory precursor cells following an acute infection by analyzing single-cell RNA-seq data that contained CD8 T cells collected during the postinfection expansion phase. We used different tools to reconstruct the developmental trajectory that CD8 T cells followed after activation. Cells that exhibited a memory precursor signature were identified and positioned on this trajectory. We found that these memory precursors are generated continuously with increasing numbers arising over time. Similarly, expression of genes associated with effector functions was also found to be raised in memory precursors at later time points. The ability of cells to enter quiescence and differentiate into memory cells was confirmed by BrdU pulse-chase experiment in vivo. Analysis of cell counts indicates that the vast majority of memory cells are generated at later time points from cells that have extensively divided.Entities:
Keywords: Bioinformatics; Cell; Cell biology; Immunology
Year: 2022 PMID: 36065187 PMCID: PMC9440290 DOI: 10.1016/j.isci.2022.104927
Source DB: PubMed Journal: iScience ISSN: 2589-0042