Upregulation of osteopontin expression is involved in the development of nonalcoholic steatohepatitis in a dietary murine model

Sahai, Atul; Malladi, Padmini; Melín-Aldana, Héctor; Green, Richard M.; Whitington, Peter F.

doi:10.1152/ajpgi.00002.2004

Cited by 167 publications

(186 citation statements)

References 49 publications

Supporting

Mentioning

158

Contrasting

Unclassified

Order By: Relevance

“…In conclusion, although the pro-fibrogenic effects of OPN have been demonstrated in several tissues including the liver, 17,[26][27][28][29] the role of OPN in the resolution of liver fibrosis was not explored until now. This study suggests that deletion of the Opn gene induces faster removal of fibrillar collagen-I after chronic liver injury likely due to a direct action on TIMP-1 expression and to less activated HSCs.…”

Section: Opn and Fibrosis Resolutionmentioning

confidence: 99%

Osteopontin delays resolution of liver fibrosis

Leung

Wang

Kitamura

et al. 2013

Laboratory Investigation

View full text Add to dashboard Cite

To date, considerable progress has been made both in the mechanisms driving liver fibrosis and in the prevention of disease progression. Resolution of liver fibrosis is an emerging field in hepatology; yet, the mediators involved remain elusive. Earlier work from our laboratory demonstrated that the matricellular cytokine osteopontin (OPN) is pro-fibrogenic by promoting hepatic stellate cell (HSC) activation and extracellular matrix (ECM) deposition in vitro and in vivo and specifically by governing fibrillar collagen-I expression, the key pro-fibrogenic protein. Here we hypothesized that OPN could also delay the resolution of liver fibrosis by sustaining collagen-I synthesis or by preventing its degradation. To demonstrate this, wild-type (WT) and OPN-knockout (Opn À / À ) mice were administered thioacetamide (TAA) in the drinking water for 4 months. Half of the mice were killed at 4 months to assess the extent of fibrosis at the peak of injury, and the rest of the mice were killed 2 months after TAA withdrawal to determine the rate of fibrosis resolution. Following TAA cessation, livers from Opn À / À mice showed no centrilobular and parenchymal necrosis along with faster ECM remodeling than WT mice. The latter was quantified by less fibrillar collagen-I immunostaining. Western blot analysis demonstrated a significant decrease in fibrillar collagen-I and in tissue inhibitor of metalloproteinase-1 (TIMP-1) in Opn À / À mice undergoing fibrosis resolution compared with WT mice. In conclusion, these results suggest that OPN delays liver fibrosis resolution due to sustained fibrillar collagen-I deposition; hence, inhibiting OPN could be an effective therapeutic strategy for resolving liver fibrosis.

show abstract

Section: Opn and Fibrosis Resolutionmentioning

confidence: 99%

Osteopontin delays resolution of liver fibrosis

Leung

Wang

Kitamura

et al. 2013

Laboratory Investigation

View full text Add to dashboard Cite

show abstract

“…OPN is also known to play an important role in a variety of inflammatory diseases like glomerular nephritis Giachelli and Steitz, 2000;O'Regan and Berman, 2000), inflammation during CCl 4 induced hepatotoxicity (Kawashima et al, 1999), puromycin-induced toxicity ) and in non-alcoholic steatohepatitis (Sahai et al, 2004). The role of OPN in inflammation has been confirmed in in vivo studies, where rats treated with neutralizing OPN antibody following induction of experimental crescentic glomerulonephritis had substantially decreased accumulation of renal interstitial macrophages as compared to the controls (Yu et al, 1998).…”

Section: Introductionmentioning

confidence: 93%

The Temporal Expression of Osteopontin (SPP-1) in the Rodent Model of Alcoholic Steatohepatitis: A Potential Biomarker

Banerjee¹,

Burghardt

Johnson

et al. 2006

Toxicol Pathol

View full text Add to dashboard Cite

Previous studies from our laboratory have shown that osteopontin (OPN) mediates neutrophil infiltration into the liver in a rodent model of alcoholic steatohepatitis (ASH). The objective of this study was to investigate the temporal and spatial pattern of hepatic OPN mRNA and protein expression during the progression of alcoholic liver disease. OPN mRNA and protein expression were evaluated using real time PCR, in situ hybridization, Western blot and immunohistochemistry respectively. ASH was induced in male Sprague-Dawley rats by feeding EtOH-containing Lieber-DeCarli diet for 6 weeks, followed by a single injection of lipopolysaccharide (LPS, 10 mg/kg, ip). Rats were sacrificed 2-, 12-and 24-hour post LPS injection. A progressive induction of OPN mRNA was observed that preceded hepatic neutrophil infiltration and the increase in OPN mRNA correlated with increases in OPN protein expression. OPN mRNA was localized primarily to the biliary epithelium. The data indicates that OPN is transcribed and translated within the biliary epithelium. These findings suggest a potential role of OPN as an early biomarker in predicting inflammatory liver diseases such as ASH.

show abstract

“…Conflicting results exist, however, with regard to the role of this chemokine in the development of liver fibrosis. Whereas liver fibrosis was reduced in osteopontin knockout mice fed a methionine/ choline-deficient diet to model nonalcoholic steatohepatitis, liver fibrosis was not reduced in mice subjected to bile duct ligation [48,49]. In addition, treatment of these mice chronically with carbon tetrachloride resulted in enhanced liver fibrosis, which may have resulted from increased liver injury in these mice [50].…”

Section: Mediators That Stimulate Hsc Chemotaxismentioning

confidence: 98%

Phenotypic Changes in Hepatic Stellate Cells in Response to Toxic Liver Injury

Copple

2014

Curr Pathobiol Rep

View full text Add to dashboard Cite

Hepatic stellate cells (HSCs) are the main extracellular matrix-producing cell type in the liver. These cells exist in a quiescent state in normal liver and an activated state in damaged liver. During quiescence, HSCs store and release various retinoids. After injury to the liver, however, various protein and non-protein mediators are released from cells that stimulate HSCs to differentiate into myofibroblasts, a process termed activation. Activated HSCs begin to express a-smooth muscle actin and migrate to sites of injury through chemotaxis. Within the damaged region of liver, these cells become contractile and produce growth factors that promote hepatocyte replication and angiogenesis, produce extracellular matrix that forms the scaffold for liver repair, and produce proteins that modulate immune cell function. Once liver repair is complete and liver function is restored, HSCs revert back to a quiescent phenotype or die by apoptosis. If liver injury becomes chronic, however, these processes persist resulting in the formation of an extensive scar (i.e., fibrosis) that ultimately leads to liver failure. Because of the importance of these cells to the development of liver fibrosis, there has been extensive research into understanding the mechanisms that drive HSC activation after injury and the mechanisms that regulate reversion of these cells back to quiescence after resolution of injury. In addition, there has been great interest in identifying the various functions of HSCs after acute and chronic injury. The aim of this review is to briefly discuss the phenotypic changes that occur in HSCs after acute and chronic liver injury and to highlight some of the important functions of these cells during repair of the liver.

show abstract

Upregulation of osteopontin expression is involved in the development of nonalcoholic steatohepatitis in a dietary murine model

Cited by 167 publications

References 49 publications

Osteopontin delays resolution of liver fibrosis

Osteopontin delays resolution of liver fibrosis

The Temporal Expression of Osteopontin (SPP-1) in the Rodent Model of Alcoholic Steatohepatitis: A Potential Biomarker

Phenotypic Changes in Hepatic Stellate Cells in Response to Toxic Liver Injury

Contact Info

Product

Resources

About