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Publication : Vaccine-elicited IL-1R signaling results in Th17 TRM-mediated immunity.

First Author  Hoffmann JP Year  2024
Journal  Commun Biol Volume  7
Issue  1 Pages  433
PubMed ID  38594380 Mgi Jnum  J:348260
Mgi Id  MGI:7620625 Doi  10.1038/s42003-024-06138-0
Citation  Hoffmann JP, et al. (2024) Vaccine-elicited IL-1R signaling results in Th17 TRM-mediated immunity. Commun Biol 7(1):433
abstractText  Lung tissue resident memory (TRM) cells are thought to play crucial roles in lung host defense. We have recently shown that immunization with the adjuvant LTA1 (derived from the A1 domain of E. coli heat labile toxin) admixed with OmpX from K. pneumoniae can elicit antigen specific lung Th17 TRM cells that provide serotype independent immunity to members of the Enterobacteriaceae family. However, the upstream requirements to generate these cells are unclear. Single-cell RNA-seq showed that vaccine-elicited Th17 TRM cells expressed high levels of IL-1R1, suggesting that IL-1 family members may be critical to generate these cells. Using a combination of genetic and antibody neutralization approaches, we show that Th17 TRM cells can be generated independent of caspase-1 but are compromised when IL-1alpha is neutralized. Moreover IL-1alpha could serve as a molecular adjuvant to generate lung Th17 TRM cells independent of LTA1. Taken together, these data suggest that IL-1alpha plays a major role in vaccine-mediated lung Th17 TRM generation.
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