Progranulin prevents regulatory NK cell cytotoxicity against antiviral T cells
Anfei Huang, Prashant V. Shinde, Jun Huang, Tina Senff, Haifeng C. Xu, Cassandra Margotta, Dieter Häussinger, Thomas E. Willnow, Jinping Zhang, Aleksandra A. Pandyra, Jörg Timm, Sascha Weggen, Karl S. Lang, Philipp A. Lang
Anfei Huang, Prashant V. Shinde, Jun Huang, Tina Senff, Haifeng C. Xu, Cassandra Margotta, Dieter Häussinger, Thomas E. Willnow, Jinping Zhang, Aleksandra A. Pandyra, Jörg Timm, Sascha Weggen, Karl S. Lang, Philipp A. Lang
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Research Article Immunology Infectious disease

Progranulin prevents regulatory NK cell cytotoxicity against antiviral T cells

Abstract

`NK cell–mediated regulation of antigen-specific T cells can contribute to and exacerbate chronic viral infection, but the protective mechanisms against NK cell–mediated attack on T cell immunity are poorly understood. Here, we show that progranulin (PGRN) can reduce NK cell cytotoxicity through reduction of NK cell expansion, granzyme B transcription, and NK cell–mediated lysis of target cells. Following infection with the lymphocytic choriomeningitis virus (LCMV), PGRN levels increased — a phenomenon dependent on the presence of macrophages and type I IFN signaling. Absence of PGRN in mice (Grn–/–) resulted in enhanced NK cell activity, increased NK cell–mediated killing of antiviral T cells, reduced antiviral T cell immunity, and increased viral burden, culminating in increased liver immunopathology. Depletion of NK cells restored antiviral immunity and alleviated pathology during infection in Grn–/– mice. In turn, PGRN treatment improved antiviral T cell immunity. Taken together, we identified PGRN as a critical factor capable of reducing NK cell–mediated attack of antiviral T cells.

Authors

Anfei Huang, Prashant V. Shinde, Jun Huang, Tina Senff, Haifeng C. Xu, Cassandra Margotta, Dieter Häussinger, Thomas E. Willnow, Jinping Zhang, Aleksandra A. Pandyra, Jörg Timm, Sascha Weggen, Karl S. Lang, Philipp A. Lang

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Figure 6

PGRN competent CD8+ T cells cannot restore antiviral immunity in Grn–/– mice.

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PGRN competent CD8+ T cells cannot restore antiviral immunity in Grn–/– ...
A total of 3000 negatively sorted P14+ (TCR transgenic CD8+ T cells recognizing the LCMV epitope gp33) T cells were transferred into WT and Grn–/– mice followed by infection with 2 × 106 pfu LCMV-WE. (A) The absolute numbers of P14+ T cells were determined at the indicated time points after infection (n = 6). (B) Virus titers from spleen, liver, lung, kidney, spinal cord (SC), and brain tissue were determined at day 12 after infection (n = 6). (C) Serum ALT (left panel) and AST (right panel) activities were examined at the indicated time points after infection (n = 6). (D) Sections of snap-frozen liver tissue (day 12) were stained with α-smooth muscle actin (α-SMA) antibodies (n = 3). Right panel indicates quantification of fluorescence intensity. Scale bars: 100 μm. Data show mean ± SEM. Each symbol represents an individual mouse. P values calculated by 2-way ANOVA (A and C) and Student’s t test (B and D), *P < 0.05; **P < 0.001; ****P < 0.0001.