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Effector TH17 Cells Give Rise to Long-Lived TRM Cells that Are Essential for an Immediate Response against Bacterial Infection

Authors :
Casey T. Weaver
João Pereira
Yuval Kluger
Piotr Bielecki
Monika S. Kowalczyk
Daniel H. Kaplan
Jun Zhao
Jun Siong Low
Will Bailis
Richard A. Flavell
Enric Esplugues
Maria Carolina Amezcua Vesely
Nicola Gagliani
Christian C. D. Harman
Hao Xu
Paris Pallis
Lina Kroehling
Paula Licona-Limón
Padmini S. Pillai
Norifumi Iijima
Akiko Iwasaki
Ruaidhri Jackson
Source :
Cell. 178:1176-1188.e15
Publication Year :
2019
Publisher :
Elsevier BV, 2019.

Abstract

Summary Adaptive immunity provides life-long protection by generating central and effector memory T cells and the most recently described tissue resident memory T (TRM) cells. However, the cellular origin of CD4 TRM cells and their contribution to host defense remain elusive. Using IL-17A tracking-fate mouse models, we found that a significant fraction of lung CD4 TRM cells derive from IL-17A-producing effector (TH17) cells following immunization with heat-killed Klebsiella pneumonia (Kp). These exTH17 TRM cells are maintained in the lung by IL-7, produced by lymphatic endothelial cells. During a memory response, neither antibodies, γδ T cells, nor circulatory T cells are sufficient for the rapid host defense required to eliminate Kp. Conversely, using parabiosis and depletion studies, we demonstrated that exTH17 TRM cells play an important role in bacterial clearance. Thus, we delineate the origin and function of airway CD4 TRM cells during bacterial infection, offering novel strategies for targeted vaccine design.

Details

ISSN :
00928674
Volume :
178
Database :
OpenAIRE
Journal :
Cell
Accession number :
edsair.doi...........374ea7f3b10c3529346615d41eecc4c3
Full Text :
https://doi.org/10.1016/j.cell.2019.07.032