NKT-associated hedgehog and osteopontin drive fibrogenesis in non-alcoholic fatty liver disease

Syn, Wing Kin; Agboola, Kolade M.; Swiderska, Marzena; Michelotti, Gregory A.; Liaskou, Evaggelia; Pang, Herbert; Xie, Guanhua; Philips, George; Chan, Isaac S.; Karaca, Gamze; Pereira, Thiago A.; Chen, Yuping; Mi, Zhiyong; Kuo, Paul C.; Choi, Steve S.; Guy, Cynthia D.; Abdelmalek, Manal F.; Diehl, Anna Mae

doi:10.1136/gutjnl-2011-301857

Cited by 231 publications

(200 citation statements)

References 38 publications

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“…Prior studies have suggested hepatic endothelium as the major source of CXCL16 in the liver in homeostasis (15), and cholangiocyte-derived CXCL16, secreted following Hedgehogpathway-dependent crosstalk with HSC, as a strong stimulus for NKT cell migration in injury (31,32). In our study, we could clearly demonstrate that also monocyte-derived inflammatory macrophages and resident Kupffer cells (defined as reported in Ref.…”

Section: Discussionsupporting

confidence: 74%

Chemokine Receptor CXCR6-Dependent Hepatic NK T Cell Accumulation Promotes Inflammation and Liver Fibrosis

Wehr

Baeck

Heymann

et al. 2013

The Journal of Immunology

227

198

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Chronic liver injury characteristically results in hepatic inflammation, which represents a prerequisite for organ fibrosis. Although NKT cells are abundantly present in liver and involved in hepatic inflammation, molecular mechanisms of their recruitment in liver fibrosis remained elusive. We hypothesized that chemokine receptor CXCR6 and its ligand CXCL16 control NKT cell migration and functionality in liver fibrosis. In patients with chronic liver diseases (n = 58), CXCR6 and CXCL16 expression was intrahepatically upregulated compared with controls. In murine liver, Cxcl16 was strongly expressed by endothelium and macrophages, whereas lymphocyte populations (NKT, NK, CD4 T, CD8 T cells) expressed CXCR6. Intravital two-photon microscopy imaging of Cxcr6+/gfp and Cxcr6gfp/gfp mice and chemotaxis studies in vitro revealed that CXCR6 specifically controls hepatic NKT cell accumulation during the early response upon experimental liver damage. Hepatic invariant NKT cells expressed distinct proinflammatory cytokines including IFN-γ and IL-4 upon injury. CXCR6-deficient mice were protected from liver fibrosis progression in two independent experimental models. Macrophage infiltration and protein levels of inflammatory cytokines IFN-γ, TNF-α, and IL-4 were also reduced in fibrotic livers of Cxcr6−/− mice, corroborating that hepatic NKT cells provide essential cytokine signals perpetuating hepatic inflammation and fibrogenesis. Adoptive transfer of NKT cells, but not CD4 T cells, isolated from wild type livers restored hepatic fibrosis in Cxcr6−/− mice upon experimental steatohepatitis. Our results demonstrate that hepatic NKT cells accumulate CXCR6-dependent early upon injury, thereby accentuating the inflammatory response in the liver and promoting hepatic fibrogenesis. Interfering with CXCR6/CXCL16 might therefore bear therapeutic potential in liver fibrosis.

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Section: Discussionsupporting

confidence: 74%

Chemokine Receptor CXCR6-Dependent Hepatic NK T Cell Accumulation Promotes Inflammation and Liver Fibrosis

Wehr

Baeck

Heymann

et al. 2013

The Journal of Immunology

227

198

View full text Add to dashboard Cite

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“…OPN also delays liver fibrosis resolution due to sustained fibrillar collagen-I deposition in mice after thioacetamide-induced fibrosis [7] . Recently, plasma OPN levels have been found to predict liver fibrosis in various chronic liver diseases, such as NASH [11] , alcoholic liver disease [12] , and chronic viral hepatitis B [13] and C [14] . Pereira et al [21] have also demonstrated that OPN secretion could be stimulated by Schistosoma mansoni and that serum OPN levels correlated with splenic vein pressure and liver fibrosis stage in patients with schistosomiasis.…”

Section: Discussionmentioning

confidence: 99%

“…In fact, plasma OPN levels have been found to be significantly elevated in patients with liver cirrhosis and HCC compared to those without HCC [10] . Recently, plasma OPN levels were shown to predict liver fibrosis in various chronic liver diseases, such as non-alcoholic steatohepatitis [11] , alcoholic liver disease [12] , and chronic viral hepatitis B [13] and C [14] . As OPN levels correlate significantly with the fibrosis stage in alcohol-induced liver disease [12] , it follows that OPN levels could be related to the degree of portal hypertension and, hence, serve as a surrogate non-invasive marker of portal hypertension.…”

Section: Introductionmentioning

confidence: 99%

Osteopontin: A non-invasive parameter of portal hypertension and prognostic marker of cirrhosis

Brůha

Jáchymová

Petrtýl

et al. 2016

WJG

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“…With the exception of infant fibrosis (biliary atresia, Caroli's disease, congenital hepatic fibrosis) and adult primary biliary cirrhosis (PBC), primary sclerosing cholangitis (PSC), and secondary biliary fibrosis, all liver diseases of other etiologies, once advanced, develop into a portal fibrosis with proliferation of biliary progenitors, especially when excessive hepatocyte apoptosis forces the stem cell niche to produce biliary progenitors. These biliary progenitors are more resistant to enhanced oxidative stress and hepatocyte death, such as induced by ASH, NASH, or severe post-transplant hepatitis C (55)(56)(57)(58)(59)(60). Drugs aimed at the biliary fibrogenic progenitors are effective antifibrotic agents in rodent biliary and advanced non-biliary fibrosis.…”

Section: Figurementioning

confidence: 99%

Evolving therapies for liver fibrosis

Schuppan

Kim²

2013

J. Clin. Invest.

533

529

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Fibrosis is an intrinsic response to chronic injury, maintaining organ integrity when extensive necrosis or apoptosis occurs. With protracted damage, fibrosis can progress toward excessive scarring and organ failure, as in liver cirrhosis. To date, antifibrotic treatment of fibrosis represents an unconquered area for drug development, with enormous potential but also high risks. Preclinical research has yielded numerous targets for antifibrotic agents, some of which have entered early-phase clinical studies, but progress has been hampered due to the relative lack of sensitive and specific biomarkers to measure fibrosis progression or reversal. Here we focus on antifibrotic approaches for liver that address specific cell types and functional units that orchestrate fibrotic wound healing responses and have a sound preclinical database or antifibrotic activity in early clinical trials. We also touch upon relevant clinical study endpoints, optimal study design, and developments in fibrosis imaging and biomarkers.

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NKT-associated hedgehog and osteopontin drive fibrogenesis in non-alcoholic fatty liver disease

Cited by 231 publications

References 38 publications

Chemokine Receptor CXCR6-Dependent Hepatic NK T Cell Accumulation Promotes Inflammation and Liver Fibrosis

Chemokine Receptor CXCR6-Dependent Hepatic NK T Cell Accumulation Promotes Inflammation and Liver Fibrosis

Osteopontin: A non-invasive parameter of portal hypertension and prognostic marker of cirrhosis

Evolving therapies for liver fibrosis

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