Kidney-resident innate-like memory γδ T cells control chronic Staphylococcus aureus infection of mice.
Tabea BertramDaniel ReimersNiels C LoryConstantin SchmidtJoanna SchmidLisa C HeinigPeter BradtkeGuido RattayStephanie ZielinskiMalte HellmigPatricia BartschHolger RohdeSarah NuñezMariana V RosemblattMaría Rosa BonoNicola GaglianiInga SandrockUlf PanzerChristian F KrebsCatherine Meyer-SchwesingerImmo PrinzHans-Willi MittrückerPublished in: Proceedings of the National Academy of Sciences of the United States of America (2022)
γδ T cells are involved in the control of Staphylococcus aureus infection, but their importance in protection compared to other T cells is unclear. We used a mouse model of systemic S. aureus infection associated with high bacterial load and persistence in the kidney. Infection caused fulminant accumulation of γδ T cells in the kidney. Renal γδ T cells acquired tissue residency and were maintained in high numbers during chronic infection. At day 7, up to 50% of renal γδ T cells produced IL-17A in situ and a large fraction of renal γδ T cells remained IL-17A + during chronic infection. Controlled depletion revealed that γδ T cells restricted renal S. aureus replication in the acute infection and provided protection during chronic renal infection and upon reinfection. Our results demonstrate that kidney-resident γδ T cells are nonredundant in limiting local S. aureus growth during chronic infection and provide enhanced protection against reinfection.