Neuroprotection against ischemic stroke requires a specific class of early responder T cells in mice

DOI

10.1172/JCI157678

Authors

Wei Cai, University of Pittsburgh School of Medicine
Ligen Shi, University of Pittsburgh School of Medicine
Jingyan Zhao, University of Pittsburgh School of Medicine
Fei Xu, University of Pittsburgh School of Medicine
Connor Dufort, University of Pittsburgh School of Medicine
Qing Ye, University of Pittsburgh School of Medicine
Tuo Yang, University of Pittsburgh School of Medicine
Xuejiao Dai, University of Pittsburgh School of Medicine
Junxuan Lyu, University of Pittsburgh School of Medicine
Chenghao Jin, University of Pittsburgh School of Medicine
Hongjian Pu, University of Pittsburgh School of Medicine
Fang Yu, University of Pittsburgh School of Medicine
Sulaiman Hassan, University of Pittsburgh School of Medicine
Zeyu Sun, University of Pittsburgh School of Medicine
Wenting Zhang, University of Pittsburgh School of Medicine
T. Kevin Hitchens, University of Pittsburgh School of Medicine
Yejie Shi, University of Pittsburgh School of Medicine
Angus W. Thomson, University of Pittsburgh Medical Center
Rehana K. Leak, Duquesne University
Xiaoming Hu, University of Pittsburgh School of Medicine
Jun Chen, University of Pittsburgh School of Medicine

Document Type

Journal Article

Publication Date

8-1-2022

Publication Title

Journal of Clinical Investigation

Volume

132

Issue

15

ISSN

219738

Abstract

Immunomodulation holds therapeutic promise against brain injuries, but leveraging this approach requires a precise understanding of mechanisms. We report that CD8+CD122+CD49dlo T regulatory-like cells (CD8+ TRLs) are among the earliest lymphocytes to infiltrate mouse brains after ischemic stroke and temper inflammation; they also confer neuroprotection. TRL depletion worsened stroke outcomes, an effect reversed by CD8+ TRL reconstitution. The CXCR3/CXCL10 axis served as the brain-homing mechanism for CD8+ TRLs. Upon brain entry, CD8+ TRLs were reprogrammed to upregulate leukemia inhibitory factor (LIF) receptor, epidermal growth factor-like transforming growth factor (ETGF), and interleukin 10 (IL-10). LIF/LIF receptor interactions induced ETGF and IL-10 production in CD8+ TRLs. While IL-10 induction was important for the antiinflammatory effects of CD8+ TRLs, ETGF provided direct neuroprotection. Poststroke intravenous transfer of CD8+ TRLs reduced infarction, promoting long-term neurological recovery in young males or aged mice of both sexes. Thus, these unique CD8+ TRLs serve as early responders to rally defenses against stroke, offering fresh perspectives for clinical translation.

Open Access

Gold

Repository Citation

Cai, W., Shi, L., Zhao, J., Xu, F., Dufort, C., Ye, Q., Yang, T., Dai, X., Lyu, J., Jin, C., Pu, H., Yu, F., Hassan, S., Sun, Z., Zhang, W., Kevin Hitchens, T., Shi, Y., Thomson, A., Leak, R., Hu, X., & Chen, J. (2022). Neuroprotection against ischemic stroke requires a specific class of early responder T cells in mice. Journal of Clinical Investigation, 132 (15). https://doi.org/10.1172/JCI157678