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

Zheng Wang; Shaohua Wang; Nick P. Goplen; Chaofan Li; In Su Cheon; Qigang Dai; Su Huang; Jinjun Shan; Chaoyu Ma; Zhenqing Ye; Min Xiang; Andrew H. Limper; Eva Carmona Porquera; Jacob E. Kohlmeier; Mark H. Kaplan; Nu Zhang; Aaron J. Johnson; Robert Vassallo; Jie Sun

doi:10.1126/sciimmunol.aaw1217

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

Zheng Wang
, Shaohua Wang
, Nick P. Goplen
, Chaofan Li
, In Su Cheon
, Qigang Dai
, Su Huang
, Jinjun Shan
, Chaoyu Ma
, Zhenqing Ye
, Min Xiang
, Andrew H. Limper
, Eva Carmona Porquera
, Jacob E. Kohlmeier
, Mark H. Kaplan
, Nu Zhang
, Aaron J. Johnson
, Robert Vassallo
, Jie Sun

Research output: Contribution to journal › Article › peer-review

109 Scopus citations

Abstract

CD8⁺ tissue-resident memory T (T_RM) cells provide frontline immunity in mucosal tissues. The mechanisms regulating CD8⁺ T_RM maintenance, heterogeneity, and protective and pathological functions are largely elusive. Here, we identify a population of CD8⁺ T_RM cells that is maintained by major histocompatibility complex class I (MHC-I) signaling, and CD80 and CD86 costimulation after acute influenza infection. These T_RM 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 T_RM 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 T_RM cells at the memory phase. Our data indicate that T_RM cell exhaustion is the result of a tissue-specific cellular adaptation that balances fibrotic sequelae with protective immunity.

Original language	English (US)
Article number	eaaw1217
Journal	Science Immunology
Volume	4
Issue number	36
DOIs	https://doi.org/10.1126/sciimmunol.aaw1217
State	Published - 2019
Externally published	Yes

Bibliographical note

Publisher Copyright:
Copyright © 2019 The Authors, some rights reserved; exclusive licensee American Association for the Advancement of Science. No claim to original U.S. Government Works

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

SDG 3 Good Health and Well-being

Publisher link

10.1126/sciimmunol.aaw1217

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Cite this

Wang, Z., Wang, S., Goplen, N. P., Li, C., Cheon, I. S., Dai, Q., Huang, S., Shan, J., Ma, C., Ye, Z., Xiang, M., Limper, A. H., Porquera, E. C., Kohlmeier, J. E., Kaplan, M. H., Zhang, N., Johnson, A. J., Vassallo, R., & Sun, J. (2019). PD-1^hi CD8⁺ resident memory T cells balance immunity and fibrotic sequelae. Science Immunology, 4(36), Article eaaw1217. https://doi.org/10.1126/sciimmunol.aaw1217

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title = "PD-1hi CD8+ resident memory T cells balance immunity and fibrotic sequelae",

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.",

author = "Zheng Wang and Shaohua Wang and Goplen, \{Nick P.\} and Chaofan Li and Cheon, \{In Su\} and Qigang Dai and Su Huang and Jinjun Shan and Chaoyu Ma and Zhenqing Ye and Min Xiang and Limper, \{Andrew H.\} and Porquera, \{Eva Carmona\} and Kohlmeier, \{Jacob E.\} and Kaplan, \{Mark H.\} and Nu Zhang and Johnson, \{Aaron J.\} and Robert Vassallo and Jie Sun",

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language = "English (US)",

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AU - Wang, Zheng

AU - Wang, Shaohua

AU - Goplen, Nick P.

AU - Li, Chaofan

AU - Cheon, In Su

AU - Dai, Qigang

AU - Huang, Su

AU - Shan, Jinjun

AU - Ma, Chaoyu

AU - Ye, Zhenqing

AU - Xiang, Min

AU - Limper, Andrew H.

AU - Porquera, Eva Carmona

AU - Kohlmeier, Jacob E.

AU - Kaplan, Mark H.

AU - Zhang, Nu

AU - Johnson, Aaron J.

AU - Vassallo, Robert

AU - Sun, Jie

PY - 2019

Y1 - 2019

N2 - 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.

AB - 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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