CD8+ T cells with an intraepithelial phenotype upregulate cytotoxic function upon influenza infection in human lung
Berber Piet, … , René A.W. van Lier, René E. Jonkers
Berber Piet, … , René A.W. van Lier, René E. Jonkers
Published May 2, 2011
Citation Information: J Clin Invest. 2011;121(6):2254-2263. https://doi.org/10.1172/JCI44675.
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CD8+ T cells with an intraepithelial phenotype upregulate cytotoxic function upon influenza infection in human lung

Abstract

The human lung T cell compartment contains many CD8+ T cells specific for respiratory viruses, suggesting that the lung is protected from recurring respiratory infections by a resident T cell pool. The entry site for respiratory viruses is the epithelium, in which a subset of lung CD8+ T cells expressing CD103 (αE integrin) resides. Here, we determined the specificity and function of CD103+CD8+ T cells in protecting human lung against viral infection. Mononuclear cells were isolated from human blood and lung resection samples. Variable numbers of CD103+CD8+ T cells were retrieved from the lung tissue. Interestingly, expression of CD103 was seen only in lung CD8+ T cells specific for influenza but not in those specific for EBV or CMV. CD103+ and influenza-reactive cells preferentially expressed NKG2A, an inhibitor of CD8+ T cell cytotoxic function. In contrast to CD103–CD8+ T cells, most CD103+CD8+ cells did not contain perforin or granzyme B. However, they could quickly upregulate these cytotoxic mediators when exposed to a type I IFN milieu or via contact with their specific antigen. This mechanism may provide a rapid and efficient response to influenza infection, without inducing cytotoxic damage to the delicate epithelial barrier.

Authors

Berber Piet, Godelieve J. de Bree, Barbara S. Smids-Dierdorp, Chris M. van der Loos, Ester B.M. Remmerswaal, Jan H. von der Thüsen, Jan M.W. van Haarst, Jan P. Eerenberg, Anja ten Brinke, Wim van der Bij, Wim Timens, René A.W. van Lier, René E. Jonkers

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Figure 3

Lung CD103+CD8+ T cells are CD45R0+ effector or memory cells.

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Lung CD103+CD8+ T cells are CD45R0+ effector or memory cells. Differ...
Differentiation stages of the CD8+ T cells within the CD103+ and CD103 cell fractions as assessed by flow cytometry. Naive cells were defined as CD27+CD45R0, memory cells were defined as CD27+CD45R0+, and effector cells were defined as CD27CD45R0±. (A) Representative FACS plots for CD103+ and CD103CD8+ T cells. Dot plots are gated on CD3+CD8+CD103+ cells among live lymphocytes or on the CD3+CD8+CD103 cells among live lymphocytes. Numbers indicate the percentages of CD3+CD8+CD103+ or CD3+CD8+CD103 cells that are located within each quadrant. (B) Naive CD8+ T cells (CD27+CD45R0), memory CD8+ T cells (CD27+CD45R0+), effector/memory (EM) CD8+ T cells (CD27CD45R0±), and CD45R0CD8+ T cells as percentages of total CD103+ and CD103CD8+ T cell fractions (n = 28). ***P < 0.0001.