Ly6Chi monocytes regulate T cell responses in viral hepatitis
Jiangao Zhu, Huiyao Chen, Xiaopei Huang, Songfu Jiang, Yiping Yang
Jiangao Zhu, Huiyao Chen, Xiaopei Huang, Songfu Jiang, Yiping Yang
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Research Article Immunology Virology

Ly6Chi monocytes regulate T cell responses in viral hepatitis

Abstract

Viral hepatitis remains a global health challenge despite recent progress in the development of more effective therapies. Although virus-specific CD8+ and CD4+ T cell responses are essential for viral clearance, it remains largely unknown what regulates T cell–mediated viral clearance. Thus, a better understanding of the regulation of anti-viral T cell immunity would be critical for the design of more effective therapies for viral hepatitis. Using a model of adenovirus-induced hepatitis, here we showed that adenoviral infection induced recruitment of Ly6Chi monocytes to the liver in a CCR2-dependent manner. These recruited Ly6Chi monocytes suppressed CD8+ and CD4+ T cell responses to adenoviral infection, leading to a delay in viral clearance. In vivo depletion of Ly6Chi monocytes markedly enhanced anti-viral T cell responses and promoted viral clearance. Mechanistically, we showed that induction of iNOS and the production of NO by Ly6Chi monocytes are critical for the suppression of T cell responses. In addition, a contact-dependent mechanism mediated by PD-1 and PD-L1 interaction is also required for T cell suppression by Ly6Chi monocytes. These findings suggest a critical role for Ly6Chi monocytes in the regulation of T cell immunity in viral hepatitis and may provide new insights into development of more effective therapies for treating viral hepatitis based on targeting the immunosuppressing monocytes.

Authors

Jiangao Zhu, Huiyao Chen, Xiaopei Huang, Songfu Jiang, Yiping Yang

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Figure 2

Depletion of monocytes leads to enhanced T cell proliferation in response to adenoviral infection in vivo.

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Depletion of monocytes leads to enhanced T cell proliferation in respons...
C57BL/6 mice were infected with recombinant adenovirus encoding LacZ (Ad) intravenously on day 0 or left uninfected (Naive). Some Ad-infected mice were also treated with 100 μg of gemcitabine hydrochloride (Gem) intraperitoneally on days 3 and 4 of infection with Ad. (A) At day 5 after infection, cells harvested from the spleen and liver were stained with anti-CD11b, anti-Ly6C, and anti-Ly6G and analyzed for the efficiency of monocyte depletion. (B) Mice were harvested at day 5 after infection. At 1 hour prior to harvest, 2 mg of BrdU in 200 μl PBS was injected intraperitoneally into mice. Spleen and liver tissues were harvested and the cells were stained with anti-CD4, anti-CD8, and anti-BrdU intracellularly. The percentage of BrdU-positive cells among CD4+ or CD8+ T cells is indicated. (C) The mean total numbers of CD4+ and CD8+ T cells, and BrdU-positive CD4+ and CD8+ T cells ± SEM are shown in the spleen (top) and liver (bottom) tissues. *P < 0.05, **P < 0.01, determined by a 2-tailed Student’s t test, n = 4. Results are representative of 3 independent experiments.