Journal article
Single-cell protein expression profiling resolves circulating and resident memory T cell diversity across tissues and infection contexts
M Evrard, E Becht, R Fonseca, A Obers, SL Park, N Ghabdan-Zanluqui, J Schroeder, SN Christo, D Schienstock, J Lai, TN Burn, A Clatch, IG House, P Beavis, A Kallies, F Ginhoux, SN Mueller, R Gottardo, EW Newell, LK Mackay
Immunity | CELL PRESS | Published : 2023
Abstract
Memory CD8+ T cells can be broadly divided into circulating (TCIRCM) and tissue-resident memory T (TRM) populations. Despite well-defined migratory and transcriptional differences, the phenotypic and functional delineation of TCIRCM and TRM cells, particularly across tissues, remains elusive. Here, we utilized an antibody screening platform and machine learning prediction pipeline (InfinityFlow) to profile >200 proteins in TCIRCM and TRM cells in solid organs and barrier locations. High-dimensional analyses revealed unappreciated heterogeneity within TCIRCM and TRM cell lineages across nine different organs after either local or systemic murine infection models. Additionally, we demonstrated..
View full abstractRelated Projects (2)
Grants
Awarded by Howard Hughes Medical Institute
Funding Acknowledgements
We thank Brooke Davies, Keely McDonald, and Natasha Zamudio for expert technical assistance. We thank the Melbourne Cytometry Platform from the Peter Doherty Institute for assistance with cell sorting. This work was supported by a Howard Hughes Medical Institute and Bill and Melinda Gates Foundation International Research Scholarship OPP1175796 to L.K.M. and an Australian Research Council grant DP200102753 to L.K.M. and M.E. L.K.M. is a senior medical research fellow supported by the Sylvia and Charles Viertel Charitable Foundation and an NHMRC Leadership Investigator Grant.