Type I interferons and TGF-β cooperate to induce liver fibrosis during HIV-1 infection under antiretroviral therapy
James Ahodantin, Kouki Nio, Masaya Funaki, Xuguang Zhai, Eleanor Wilson, Shyamasundaran Kottilil, Liang Cheng, Guangming Li, Lishan Su
James Ahodantin, Kouki Nio, Masaya Funaki, Xuguang Zhai, Eleanor Wilson, Shyamasundaran Kottilil, Liang Cheng, Guangming Li, Lishan Su
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Research Article AIDS/HIV Inflammation

Type I interferons and TGF-β cooperate to induce liver fibrosis during HIV-1 infection under antiretroviral therapy

Abstract

Liver diseases have become a major comorbidity health concern for people living with HIV-1 (PLWH) treated with combination antiretroviral therapy (cART). To investigate if HIV-1 infection and cART interact to lead to liver diseases, humanized mice reconstituted with progenitor cells from human fetal livers were infected with HIV-1 and treated with cART. We report here that chronic HIV-1 infection with cART induced hepatitis and liver fibrosis in humanized mice, associated with accumulation of M2-like macrophages (M2LMs), elevated TGF-β, and IFN signaling in the liver. Interestingly, IFN-I and TGF-β cooperatively activated human hepatic stellate cells (HepSCs) in vitro. Mechanistically, IFN-I enhanced TGF-β–induced SMAD2/3 activation in HepSCs. Finally, blockade of IFN-I signaling reversed HIV/cART-induced liver diseases in humanized mice. Consistent with the findings in humanized mice with HIV-1 and cART, we detected elevated markers of liver injury, M2LMs, and of IFN signaling in blood specimens from PLWH compared with those of healthy individuals. These findings identify the IFN-I/M2LM/HepSC axis in HIV/cART-induced liver diseases and suggest that inhibiting IFN-I signaling or M2LM may provide a novel therapeutic strategy for treating HIV/cART-associated liver diseases in PLWH treated with antiretroviral therapy.

Authors

James Ahodantin, Kouki Nio, Masaya Funaki, Xuguang Zhai, Eleanor Wilson, Shyamasundaran Kottilil, Liang Cheng, Guangming Li, Lishan Su

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Figure 6

Blockade of IFN-I signaling prevents HIV/cART-induced hepatic accumulation of M2-like macrophages and liver fibrosis or diseases in hu-mice.

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Blockade of IFN-I signaling prevents HIV/cART-induced hepatic accumulati...
(A) Diagram of experimental design. Blood and liver tissues from mock- and HIV-infected NRG-hu HSC mice treated with cART were analyzed at 12–13 wpi. (B–D) Assessment of the anti–IFNAR1 Ab treatment on liver immune infiltration. (B) Liver sections were costained for human CD45/CD3 (brown/red), CD68/MerTK (brown/red) by IHC (original magnification, ×20). (C) Expression of human MerTK and TGF-β was detected in the liver by RT-qPCR; data were normalized with mouse Gapdh. (D) Soluble CD163 levels were measured in the blood of hu-mice by ELISA. (E) Quantification of hyaluronic acid in the serum by ELISA. (F–H) Decrease of liver fibrosis in animals treated with anti-IFNAR1. (F) Liver sections were stained for SR and (G) collagen deposition automatically was quantified by deconvolution algorithm analysis. (H) Immunoblot and quantification of α-SMA expression in the liver. Histograms represent the SEM; bars in the scatter plots represent the median. Statistical analysis was performed with 1-way ANOVA and Turkey’s post hoc test. *P < 0.05; **P < 0.005. Conc., concentration.