Notch-mediated hepatocyte MCP-1 secretion causes liver fibrosis
Jinku Kang, Jorge Postigo-Fernandez, KyeongJin Kim, Changyu Zhu, Junjie Yu, Marica Meroni, Brent Mayfield, Alberto Bartolomé, Dianne H. Dapito, Anthony W. Ferrante Jr., Paola Dongiovanni, Luca Valenti, Remi J. Creusot, Utpal B. Pajvani
Jinku Kang, Jorge Postigo-Fernandez, KyeongJin Kim, Changyu Zhu, Junjie Yu, Marica Meroni, Brent Mayfield, Alberto Bartolomé, Dianne H. Dapito, Anthony W. Ferrante Jr., Paola Dongiovanni, Luca Valenti, Remi J. Creusot, Utpal B. Pajvani
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Research Article Gastroenterology Metabolism

Notch-mediated hepatocyte MCP-1 secretion causes liver fibrosis

Abstract

Patients with nonalcoholic steatohepatitis (NASH) have increased expression of liver monocyte chemoattractant protein-1 (MCP-1), but its cellular source and contribution to various aspects of NASH pathophysiology remain debated. We demonstrated increased liver CCL2 (which encodes MCP-1) expression in patients with NASH, and commensurately, a 100-fold increase in hepatocyte Ccl2 expression in a mouse model of NASH, accompanied by increased liver monocyte-derived macrophage (MoMF) infiltrate and liver fibrosis. To test repercussions of increased hepatocyte-derived MCP-1, we generated hepatocyte-specific Ccl2-knockout mice, which showed reduced liver MoMF infiltrate as well as decreased liver fibrosis. Forced hepatocyte MCP-1 expression provoked the opposite phenotype in chow-fed wild-type mice. Consistent with increased hepatocyte Notch signaling in NASH, we observed a close correlation between markers of Notch activation and CCL2 expression in patients with NASH. We found that an evolutionarily conserved Notch/recombination signal binding protein for immunoglobulin kappa J region binding site in the Ccl2 promoter mediated transactivation of the Ccl2 promoter in NASH diet–fed mice. Increased liver MoMF infiltrate and liver fibrosis seen in opposite gain-of-function mice was ameliorated with concomitant hepatocyte Ccl2 knockout or CCR2 inhibitor treatment. Hepatocyte Notch activation prompts MCP-1–dependent increase in liver MoMF infiltration and fibrosis.

Authors

Jinku Kang, Jorge Postigo-Fernandez, KyeongJin Kim, Changyu Zhu, Junjie Yu, Marica Meroni, Brent Mayfield, Alberto Bartolomé, Dianne H. Dapito, Anthony W. Ferrante Jr., Paola Dongiovanni, Luca Valenti, Remi J. Creusot, Utpal B. Pajvani

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Figure 3

MCP-1 loss of function reduces liver fibrosis with NASH diet for 16 weeks.

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MCP-1 loss of function reduces liver fibrosis with NASH diet for 16 week...
(A) Experimental schematic for hepatocyte-specific MCP-1-knockout mice. Male 8-week-old MCP-1fl/fl mice were transduced with AAV8-Tbg-Gfp (Control) or AAV8-Tbg-Cre to generate MCP-1ΔHep male mice, then fed with NASH diet for 16 weeks (n = 8 mice/group). (B) Gene expression for liver Ccl2 from chow- or NASH diet–fed control mice or MCP-1ΔHep male mice (n = 8 mice/group). (C) Markers of HSC activity from chow- or NASH diet–fed control mice or MCP-1ΔHep male mice (n = 8 mice/group). (D) Representative IHC image of Col1a1 protein expression from chow- or NASH diet–fed control mice or MCP-1ΔHep male mice. (E) Liver Sirius red staining and quantitation in control and MCP-1ΔHep male mice (n = 8 mice/group). Scale bars: 50 μm. All data are shown with group means ± SEM; *, P < 0.05, **, P < 0.01, ***, P < 0.001 by 1-way ANOVA followed by Tukey’s multiple comparisons test.