Plasmacytoid dendritic cells promote HIV-1–induced group 3 innate lymphoid cell depletion
Zheng Zhang, … , Fu-Sheng Wang, Lishan Su
Zheng Zhang, … , Fu-Sheng Wang, Lishan Su
Published August 24, 2015
Citation Information: J Clin Invest. 2015;125(9):3692-3703. https://doi.org/10.1172/JCI82124.
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Research Article AIDS/HIV

Plasmacytoid dendritic cells promote HIV-1–induced group 3 innate lymphoid cell depletion

Abstract

Group 3 innate lymphoid cells (ILC3s) have demonstrated roles in promoting antibacterial immunity, maintaining epithelial barrier function, and supporting tissue repair. ILC3 alterations are associated with chronic inflammation and inflammatory disease; however, the characteristics and relevant regulatory mechanisms of this cell population in HIV-1 infection are poorly understood due in part to a lack of a robust model. Here, we determined that functional human ILC3s develop in lymphoid organs of humanized mice and that persistent HIV-1 infection in this model depletes ILC3s, as observed in chronic HIV-1–infected patients. In HIV-1–infected mice, effective antiretroviral therapy reversed the loss of ILC3s. HIV-1–dependent reduction of ILC3s required plasmacytoid dendritic cells (pDCs), IFN-I, and the CD95/FasL pathway, as targeted depletion or blockade of these prevented HIV-1–induced ILC3 depletion in vivo and in vitro, respectively. Finally, we determined that HIV-1 infection induces CD95 expression on ILC3s via a pDC- and IFN-I–dependent mechanism that sensitizes ILC3s to undergo CD95/FasL-mediated apoptosis. We conclude that chronic HIV-1 infection depletes ILC3s through pDC activation, induction of IFN-I, and CD95-mediated apoptosis.

Authors

Zheng Zhang, Liang Cheng, Juanjuan Zhao, Guangming Li, Liguo Zhang, Weiwei Chen, Weiming Nie, Natalia J. Reszka-Blanco, Fu-Sheng Wang, Lishan Su

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Figure 5

Depletion of pDCs increases HIV-1 replication, but reduces HIV-1–induced immunopathogenesis.

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Depletion of pDCs increases HIV-1 replication, but reduces HIV-1–induced...
Humanized mice were infected with HIV-JRCSF for 8 weeks and were subsequently treated with 15B or cART twice every week for 6 weeks and terminated at 14 wpi (mock, n = 6; JR-CSF, n = 6; JR-CSF+cART, n = 8; JR-CSF+15B, n = 6). Splenic pDC percentages (A), plasma IFN-α (B), and HIV-1 genome RNA levels (C), and splenic hCD45+ cell counts (D) and CD4+ (E) and CD8+ T cell counts (F) were analyzed in 4 groups of mice. Data are representative of 3 independent experiments with 3 to 4 donors. Overall, for pDC percentages, P = 0.0053; P < 0.0001 (plasma IFN-α); P < 0.0001 (plasma HIV-1 load); P = 0.0009 (splenic hCD45+ cell counts); P < 0.0001 (CD4+ T cell counts); and P = 0.0022 (CD8+ T cell counts), 1-way ANOVA. *P < 0.05; **P < 0.01; ***P < 0.001, Tukey’s post-hoc test.