期刊
MUCOSAL IMMUNOLOGY
卷 15, 期 4, 页码 717-729出版社
ELSEVIER SCIENCE INC
DOI: 10.1038/s41385-022-00497-9
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资金
- People Programme (Marie Curie Actions) of the European Union's Seventh Framework Programme FP7/2007-2013/under REA grant [607690]
- Knut and Alice Wallenberg Foundation [KAW 2013.0030]
- Swedish Foundation for Strategic Research [SB12-0088]
- Swedish Cancer Foundation
- Swedish Research Council
- EU project UNISEC [LUA/ALF ALFGBG-531021]
- Lundberg foundation
- SciLife Sweden for bioinformatics analysis of the scRNAseq data
- FP7-ITN project UNIVACFLU
- FWO [G052412N]
- Belgian Federal Sciences Administration Project [BELVIR p7/45]
- Swedish Foundation for Strategic Research (SSF) [SB12-0088] Funding Source: Swedish Foundation for Strategic Research (SSF)
Intranasal immunization with CTA1-3M2e-DD stimulates M2e-specific Th17 Trm cells, which provide strong protection against influenza virus infection and tissue injury. Single-cell RNAseq analysis reveals functional diversity of these Trm cells in the lung, and the same TCR clonotype can differentiate into different subclusters with distinct functions. These findings have important implications for vaccine development against respiratory virus infections.
The fate of tissue-resident memory CD4 T cells (Trm) has been incompletely investigated. Here we show that intranasal, but not parenteral, immunization with CTA1-3M2e-DD stimulated M2e-specific Th17 Trm cells, which conferred strong protection against influenza virus infection in the lung. These cells rapidly expanded upon infection and effectively restricted virus replication as determined by CD4 T cell depletion studies. Single-cell RNAseq transcriptomic and TCR VDJ-analysis of M2e-tetramer-sorted CD4 T cells on day 3 and 8 post infection revealed complete Th17-lineage dominance (no Th1 or Tregs) with extensive functional diversity and expression of gene markers signifying mature resident Trm cells (Cd69, Nfkbid, Brd2, FosB). Unexpectedly, the same TCR clonotype hosted cells with different Th17 subcluster functions (IL-17, IL-22), regulatory and cytotoxic cells, suggesting a tissue and context-dependent differentiation of reactivated Th17 Trm cells. A gene set enrichment analysis demonstrated up-regulation of regulatory genes (Lag3, Tigit, Ctla4, Pdcd1) in M2e-specific Trm cells on day 8, indicating a tissue damage preventing function. Thus, contrary to current thinking, lung M2e-specific Th17 Trm cells are sufficient for controlling infection and for protecting against tissue injury. These findings will have strong implications for vaccine development against respiratory virus infections and influenza virus infections, in particular.
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