AUTHOR=Suarez-Ramirez Jenny E. , Chandiran Karthik , Brocke Stefan , Cauley Linda S. 

TITLE=Immunity to Respiratory Infection Is Reinforced Through Early Proliferation of Lymphoid TRM Cells and Prompt Arrival of Effector CD8 T Cells in the Lungs

JOURNAL=Frontiers in Immunology

VOLUME=10

YEAR=2019

URL=https://www.frontiersin.org/journals/immunology/articles/10.3389/fimmu.2019.01370

DOI=10.3389/fimmu.2019.01370

ISSN=1664-3224

ABSTRACT=<p>Cross-protection between serologically distinct strains of influenza A virus (IAV) is mediated by memory CD8 T cells that recognize epitopes from conserved viral proteins. Early viral control begins with activation of tissue-resident memory CD8 T cells (T<sub>RM</sub>) cells at the site of viral replication. These CD8 T cells do not act in isolation, as protection against disseminated infection is reinforced by multiple waves of effector cells (T<sub>EFF</sub>) that enter the lungs with different kinetics. To define how a protective CTL response evolves, we compared the functional properties of antiviral CD8 T cells in the respiratory tract and local lymphoid tissues. When analyzed 30 dpi, large numbers of antiviral CD8 T cells in the lungs and mediastinal lymph nodes (MLNs) expressed canonical markers of T<sub>RM</sub> cells (CD69 and/or CD103). The check point inhibitor PD-1 was also highly expressed on NP-specific CD8 T cells in the lungs, while the ratios of CD8 T cells expressing CD69 and CD103 varied according to antigen specificity. We next used <italic>in vitro</italic> experiments to identify conditions that induce a canonical T<sub>RM</sub> phenotype and found that that naïve and newly activated CD8 T cells maintain CD103 expression during culture with transforming growth factor-beta (TGFβ), while central memory CD8 T cells (T<sub>CM</sub>) do not express CD103 under similar conditions. <italic>In vivo</italic> experiments showed that the distribution of antiviral CTLs in the MLN changed when immune mice were treated with reagents that block interactions with PD-L1. Importantly, the lymphoid T<sub>RM</sub> cells were poised for early proliferation upon reinfection with a different strain of IAV and defenses in the lungs were augmented by a transient increase in numbers of T<sub>EFF</sub> cells at the site of infection. As the interval between infections increased, lymphoid T<sub>RM</sub> cells were replaced with T<sub>CM</sub> cells which proliferated with delayed kinetics and contributed to an exaggerated inflammatory response in the lungs.</p>