Antagonism of the chemokine Ccl5 ameliorates experimental liver fibrosis in mice
Marie-Luise Berres, … , Christian Trautwein, Hermann E. Wasmuth
Marie-Luise Berres, … , Christian Trautwein, Hermann E. Wasmuth
Published October 18, 2010
Citation Information: J Clin Invest. 2010;120(11):4129-4140. https://doi.org/10.1172/JCI41732.
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Research Article Hepatology

Antagonism of the chemokine Ccl5 ameliorates experimental liver fibrosis in mice

Abstract

Activation of hepatic stellate cells in response to chronic inflammation represents a crucial step in the development of liver fibrosis. However, the molecules involved in the interaction between immune cells and stellate cells remain obscure. Herein, we identify the chemokine CCL5 (also known as RANTES), which is induced in murine and human liver after injury, as a central mediator of this interaction. First, we showed in patients with liver fibrosis that CCL5 haplotypes and intrahepatic CCL5 mRNA expression were associated with severe liver fibrosis. Consistent with this, we detected Ccl5 mRNA and CCL5 protein in 2 mouse models of liver fibrosis, induced by either injection of carbon tetrachloride (CCl4) or feeding on a methionine and choline–deficient (MCD) diet. In these models, Ccl5–/– mice exhibited decreased hepatic fibrosis, with reduced stellate cell activation and immune cell infiltration. Transplantation of Ccl5-deficient bone marrow into WT recipients attenuated liver fibrosis, identifying infiltrating hematopoietic cells as the main source of Ccl5. We then showed that treatment with the CCL5 receptor antagonist Met-CCL5 inhibited cultured stellate cell migration, proliferation, and chemokine and collagen secretion. Importantly, in vivo administration of Met-CCL5 greatly ameliorated liver fibrosis in mice and was able to accelerate fibrosis regression. Our results define a successful therapeutic approach to reduce experimental liver fibrosis by antagonizing Ccl5 receptors.

Authors

Marie-Luise Berres, Rory R. Koenen, Anna Rueland, Mirko Moreno Zaldivar, Daniel Heinrichs, Hacer Sahin, Petra Schmitz, Konrad L. Streetz, Thomas Berg, Nikolaus Gassler, Ralf Weiskirchen, Amanda Proudfoot, Christian Weber, Christian Trautwein, Hermann E. Wasmuth

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Figure 7

Met-CCL5 accelerates the regression of liver fibrosis in vivo.

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Met-CCL5 accelerates the regression of liver fibrosis in vivo. (A) C57BL...
(A) C57BL/6 mice were challenged with CCl4 for 8 weeks to establish advanced liver scarring. Three days after the last the last CCl4 injection (at the peak of fibrosis), mice received either Met-CCL5 or vehicle (n = 8/group) and were assessed for fibrosis regression by histology for an overall duration of 7 days. At day 7, the mice that received Met-CCL5 displayed a significantly reduced residual fibrosis compared with the vehicle-treated group (original magnifications, ×40). (B) The difference between the groups is evidenced by a reduced Sirius red–positive area in the Met-CCL5–treated mice (*P < 0.05) and (C) by significantly lower hydroxyproline contents at the same time point during fibrosis regression (*P < 0.05). (D) Functionally, mRNA expression of Col1a1 and Timp1 is already significantly reduced at day 3, after start of Met-CCL5 or vehicle treatment (*P < 0.05).