PD-1hi CD8+ resident memory T cells balance immunity and fibrotic sequelae

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Date
2019-06-14
Authors
Wang, Zheng
Wang, Shaohua
Goplen, Nick P.
Li, Chaofan
Cheon, In Su
Dai, Qigang
Huang, Su
Shan, Jinjun
Ma, Chaoyu
Ye, Zhenqing
Xiang, Min
Limper, Andrew H.
Porquera, Eva-Carmona
Kohlmeier, Jacob E.
Kaplan, Mark H.
Zhang, Nu
Johnson, Aaron J.
Vassallo, Robert
Sun, Jie
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American English
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Microbiology and Immunology, School of Medicine
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Science Immunology
Abstract

CD8+ tissue-resident memory T (TRM) cells provide frontline immunity in mucosal tissues. The mechanisms regulating CD8+ TRM maintenance, heterogeneity, and protective and pathological functions are largely elusive. Here, we identify a population of CD8+ TRM cells that is maintained by major histocompatibility complex class I (MHC-I) signaling, and CD80 and CD86 costimulation after acute influenza infection. These TRM cells have both exhausted-like phenotypes and memory features and provide heterologous immunity against secondary infection. PD-L1 blockade after the resolution of primary infection promotes the rejuvenation of these exhausted-like TRM cells, restoring protective immunity at the cost of promoting postinfection inflammatory and fibrotic sequelae. Thus, PD-1 serves to limit the pathogenic capacity of exhausted-like TRM cells at the memory phase. Our data indicate that TRM cell exhaustion is the result of a tissue-specific cellular adaptation that balances fibrotic sequelae with protective immunity.

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B7-H1 Antigen, Immunologic Memory, Orthomyxoviridae Infections, Programmed Cell Death 1 Receptor
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CD8+ tissue-resident memory T (TRM) cells provide frontline immunity in mucosal tissues. The mechanisms regulating CD8+ TRM maintenance, heterogeneity, and protective and pathological functions are largely elusive. Here, we identify a population of CD8+ TRM cells that is maintained by major histocompatibility complex class I (MHC-I) signaling, and CD80 and CD86 costimulation after acute influenza infection. These TRM cells have both exhausted-like phenotypes and memory features and provide heterologous immunity against secondary infection. PD-L1 blockade after the resolution of primary infection promotes the rejuvenation of these exhausted-like TRM cells, restoring protective immunity at the cost of promoting postinfection inflammatory and fibrotic sequelae. Thus, PD-1 serves to limit the pathogenic capacity of exhausted-like TRM cells at the memory phase. Our data indicate that TRM cell exhaustion is the result of a tissue-specific cellular adaptation that balances fibrotic sequelae with protective immunity.
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2470-9468
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Science Immunology
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https://hdl.handle.net/1805/26026
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https://doi.org/10.1126/sciimmunol.aaw1217
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