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Query: UMLS:C0019158 (
hepatitis
)
30,205
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
Osteopontin
, a crucial factor for Th1 immune response, is expressed in stellate cells and macrophages activated in injured liver. To clarify the role of
osteopontin
in inflammatory changes in the liver, we attempted to establish transgenic mice expressing
osteopontin
in hepatocytes. Mouse
osteopontin
cDNA, cloned from concanavalin-A-stimulated spleen cells in C57BL/6 mice, was constructed into the vector containing serum amyloid-P component promoter. This construction was microinjected into fertilized eggs of C57BL/6 mice, and 4 lines of the transgenic mice were obtained. Western blotting and immunohistochemistry revealed that
osteopontin
was expressed in hepatocytes, but not in non-parenchymal cells, in the transgenic mice. The mean
osteopontin
concentrations in the liver and plasma in the mice were 13 and 2.6 times higher than those in negative littermates. Antinuclear antibody was positive in the plasma in 50% of the transgenic mice. In the transgenic mice later than 12 weeks of age, mononuclear cell infiltration in the liver developed, and these cells were positive for CD8 and HLA-DR. Plasma ALT activity was increased with focal necrosis in hepatic lobules in the transgenic mice later than 24 weeks of age. The transgenic mice expressing
osteopontin
in hepatocytes may be useful as a model of autoimmune
hepatitis
.
...
PMID:Transgenic mice expressing osteopontin in hepatocytes as a model of autoimmune hepatitis. 1504 55
Fulminant hepatitis is characterized by massive or submassive liver necrosis. Massive liver necrosis can be induced by activated macrophages infiltrating into the liver.
Osteopontin
, an extracellular matrix, is a secretory glycoprotein as well essential for Th1 immune response, contributing to macrophage activation and infiltration. To know the significance of
osteopontin
in the development of fulminant
hepatitis
, plasma
osteopontin
levels were measured in patients with fulminant
hepatitis
. The levels were significantly greater in patients with fulminant
hepatitis
than in those with acute or chronic hepatitis as well as healthy adults. Among patients with fulminant
hepatitis
except one in whom bacterial infection was complicated, plasma
osteopontin
levels were elevated especially in the patients who developed hepatic encephalopathy of grade II or more within 10 days of the disease onset, a clinical type characteristic of massive liver necrosis. Immunohistochemical examination revealed that
osteopontin
was stained in macrophages positive for CD68, a marker for macrophages, in necrotic areas of the liver in a patient with fulminant
hepatitis
. In conclusion, plasma
osteopontin
levels were elevated in patients with fulminant
hepatitis
, probably reflecting production of
osteopontin
in Kupffer cells and hepatic macrophages, which might be involved in the development of massive liver necrosis in fulminant
hepatitis
.
...
PMID:Plasma osteopontin levels in patients with fulminant hepatitis. 1528 11
Both
osteopontin
(
OPN
) and natural killer T (NKT) cells play a role in the development of immunological disorders. We examined a functional link between
OPN
and NKT cells. Concanavalin A (Con A)-induced
hepatitis
is a well-characterized murine model of T cell-mediated liver diseases. Here, we show that NKT cells secrete
OPN
, which augments NKT cell activation and triggers neutrophil infiltration and activation. Thus,
OPN
- and NKT cell-deficient mice were refractory to Con A-induced
hepatitis
. In addition, a neutralizing antibody specific for a cryptic epitope of
OPN
, exposed by thrombin cleavage, ameliorated
hepatitis
. These findings identify NKT cell-derived
OPN
as a novel target for the treatment of inflammatory liver diseases.
...
PMID:Osteopontin as a mediator of NKT cell function in T cell-mediated liver diseases. 1548 31
There have been many reports about the severity of hepatic necrosis caused by fulminant
hepatitis
; however, the relation between proliferated bile ductules and
osteopontin
(
OPN
) expression in inflamed areas in each of the clinical forms of fulminant
hepatitis
has not been described. To analyze the mechanism in the onset of fulminant
hepatitis
, we classified not only 16 autopsy cases of fulminant
hepatitis
into two clinical forms--acute and subacute--but also 3 autopsy cases of late-onset hepatic failure (LOHF) associated with fulminant
hepatitis
, and examined liver specimens by light microscopy and immunohistochemistry and also serum transaminase levels. Histopathologic study revealed that some of the proliferated bile ductules were associated directly with deteriorating hepatocytes and that bile plugs were present in the proliferated bile ductules. The value of the proliferative cell nuclear antigen labeling index (PCNA-L I) for proliferated bile ductules was very high during the acute form of fulminant
hepatitis
. Immunohistochemical analysis revealed that
OPN
expression was higher in the proliferated bile ductules of acute-form fulminant
hepatitis
than in cirrhotic and normal liver bile ducts. Transaminase levels in acute-form fulminant
hepatitis
were significantly elevated in comparison with levels in the other forms of the disease. Comparison of acute form fulminant
hepatitis
with the subacute form and LOHF showed
OPN
expression in proliferated bile ductules and serum aspartate aminotransferase (ALT)max to be decreased in the subacute form of fulminant
hepatitis
.
OPN
expression is an important marker of the degree of liver inflammation, and its regulation mechanism is very important to understanding the pathophysiology of fulminant
hepatitis
.
...
PMID:Osteopontin expression in proliferated bile ductules: the correlation with liver damage in fulminant hepatitis. 1571 59
The acquired or perinatal form of biliary atresia is a Th1 fibro-inflammatory disease affecting both the extrahepatic and intrahepatic bile ducts.
Osteopontin
(
OPN
) is a Th1 cytokine implicated in several fibro-inflammatory and autoimmune diseases. We examined the expression of
OPN
in acquired biliary atresia in comparison to normal liver and several pediatric cholestatic liver diseases. We also assessed
OPN
expression by cultured human bile duct epithelial cells. We found that liver
OPN
mRNA and protein expression were significantly increased in biliary atresia versus normal and other cholestatic diseases.
OPN
expression in biliary atresia was localized to epithelium of proliferating biliary structures (ductules and/or ducts) and bile plugs contained therein. No portal biliary
OPN
expression could be demonstrated in normal liver, syndromic biliary atresia, biliary obstruction not due to biliary atresia, and idiopathic neonatal
hepatitis
.
OPN
expression by human bile duct epithelial cells in culture was responsive to IL-2 and TNF-alpha. Our results demonstrate an up-regulation of
OPN
expression by interlobular biliary epithelium in biliary atresia, which correlates with biliary proliferation and portal fibrosis. These findings suggest a role for
OPN
in the pathogenesis of biliary atresia.
...
PMID:Expression of osteopontin correlates with portal biliary proliferation and fibrosis in biliary atresia. 1584 35
Osteopontin
(
OPN
) is a highly modified integrin-binding extracellular matrix glycophosphoprotein produced by cells of the immune system, epithelial tissue, smooth muscle cells, osteoblasts, and tumor cells. Extensive research has elucidated the pivotal role of
OPN
in cell signaling that controls inflammation, tumor progression, and metastasis.
OPN
interaction with the integrin receptors expressed on inflammatory cells through its arginine-glycine-aspartate (RGD) and non-RGD motifs promote migration and adhesion of cells. In the liver, it has been reported that hepatic Kupffer cells secrete
OPN
facilitating macrophage infiltration into necrotic areas following carbon tetrachloride liver toxicity. Recent work has highlighted the role of
OPN
in inflammatory liver diseases such as alcoholic and nonalcoholic liver disease and T-cell-mediated
hepatitis
. The role of
OPN
in hepatocellular carcinoma (HCC) has also generated significant interest, especially with regards to its role as a prognostic factor.
OPN
therefore appears to play an important role during liver inflammation and cancer. In this review we will present data to demonstrate the key role played by
OPN
in mediating hepatic inflammation (neutrophils, monocytes/macrophages, and lymphocytes) and its role in HCC. Greater understanding of the pathophysiologic role of
OPN
in hepatic inflammation and cancer may enable development of novel inflammation and cancer treatment strategies.
...
PMID:Pathophysiological role of osteopontin in hepatic inflammation, toxicity, and cancer. 1789 Jul 65
Osteopontin
(
OPN
) has been implicated in various helper T cell type 1 immunity-mediated diseases including rheumatoid arthritis (RA), multiple sclerosis (MS), Crohn's disease, and fulminant
hepatitis
. Increased expression of
OPN
has been detected in pathological foci of these diseases. RA and fulminant
hepatitis
have been successfully treated by administration of neutralizing anti-
OPN
antibody in mice. Antibody treatment may elicit side effects including allergic reactions against heterologous antibody proteins, thus necessitating humanization of antibody. To provide alternative means to neutralize
OPN
function, in this study we explored the possibility of using
OPN
small interfering RNA (siRNA) to silence
OPN
gene expression. In vitro,
OPN
siRNA efficiently silenced the expression of both exogenous and endogenous
OPN
gene. After hydrodynamic intravenous injection of
OPN
siRNA,
OPN
siRNA was efficiently delivered to the liver, which resulted in the efficient silencing of
OPN
gene expression in liver. In a murine model of concanavalin A (ConA)-induced fulminant
hepatitis
,
OPN
expression was elevated in liver and severe hepatic necrosis was induced. Importantly, after
OPN
siRNA treatment, the
OPN
expression level in liver was significantly reduced and liver tissue injury was ameliorated, as reflected by the significant reduction of serum alanine aminotransferase levels and almost normal liver histology. Thus, this study indicates that
OPN
siRNA delivery has therapeutic potential in various inflammatory diseases in which
OPN
play a critical role by silencing
OPN
gene expression in vivo.
...
PMID:Osteopontin small interfering RNA protects mice from fulminant hepatitis. 1798 93
The pathogenesis of non-alcoholic fatty liver disease (NAFLD) remains largely unknown. Here, we assessed the importance of hepatic fat accumulation on the progression of
hepatitis
. BALB/cA mice were fed with a standard diet (STD) or a high-fat and high-sucrose diet (HFHSD) for 14 days followed by intraperitoneal injection of d-galactosamine (DGalN) or vehicle. After 20-21 h, plasma and liver tissue were collected and analyzed. Alanine aminotransferase (ALT) and aspartate aminotransferase (AST) levels in plasma were increased significantly in HFHSD-fed mice treated with DGalN compared to STD-fed mice treated with DGalN. This exacerbation by the HFHSD was also observed in the plasma soluble tumor necrosis factor receptor (sTNFR) levels, and hepatic levels of reactive oxygen species (ROS) and the fibrogenic gene expression, such as tissue inhibitor of matrix metalloproteinase 1 (TIMP-1), connective tissue growth factor (CTGF) and
osteopontin
(
OPN
) in HFHSD-fed mice treated with DGalN. The triglyceride contents of the liver were significantly increased by the HFHSD. When eicosapentaenoic acid (EPA), a suppressor of sterol regulatory element binding protein 1 (SREBP-1), was administered to HFHSD-fed mice, the sensitivity of DGalN, as a result of plasma ALT and AST levels, was suppressed accompanied by reduced plasma sTNFR2 level and hepatic levels of triglyceride, ROS, and fibrogenic parameters, and by increased plasma adiponectin levels. These data suggest that the progression of steatotic liver injury closely depends on the accumulation of fat in the liver and is prevented by EPA through the suppression of the fatty liver change.
...
PMID:Suppression of hepatic fat accumulation by highly purified eicosapentaenoic acid prevents the progression of d-galactosamine-induced hepatitis in mice fed with a high-fat/high-sucrose diet. 1941 47
Immune-mediated liver diseases including autoimmune and viral hepatitis are a major health problem worldwide. In this study, we report that activation of the farnesoid X receptor (FXR), a member of the ligand-activated nuclear receptor superfamily and bile sensor highly expressed in the liver, attenuates liver injury in a model of autoimmune
hepatitis
induced by Con A. We found that FXR gene ablation results in a time-dependent increase of liver expression (up to 20-fold in a 9-mo-old mouse) of
osteopontin
, a NKT cell-derived extracellular matrix protein and immunoregulatory cytokine. In comparison to wild-type, FXR(-/-) mice are more susceptible to Con A-induced
hepatitis
and react to Con A administration by an unregulated production of
osteopontin
. Administering wild-type mice with a synthetic FXR agonist attenuated Con A-induced liver damage and liver expression of the
osteopontin
gene. By in vitro studies, we found that FXR is expressed by primarily isolated NKT cells and its ablation favors ostepontin production in response to Con A. Chromatin immunoprecipitation assay and coimmunoprecipitation experiments demonstrate that the short heterodimer partner (SHP), a nuclear receptor and FXR target, was expressed by NKT cell hybridomas and increased in response to FXR activation. FXR activates SHP that interacts with and inhibits c-Jun binding to the
osteopontin
promoter. These data indicate that in NKT cells, FXR activation causes a SHP-mediated inhibition of
osteopontin
production. These data support the notion that the bile acid sensor FXR regulates the activation of liver NKT cells.
...
PMID:The bile acid sensor farnesoid X receptor is a modulator of liver immunity in a rodent model of acute hepatitis. 1988 Apr 46
Carboxypeptidase R (CPR), also known as thrombin-activatable fibrinolysis inhibitor (TAFI), is an enzyme generated by proteolytic cleavage of its zymogen (proCPR). CPR removes the C-terminal arginine from inflammatory peptides such as C3a and C5a, bradykinin, enkephalin, and the thrombin-cleaved N-terminal fragment
osteopontin
(cleaved N-OPN). In the mouse model of concanavalin A (Con A)-induced immune-mediated fulminating
hepatitis
, cleaved N-OPN is one of the important peptides that induce the production of chemokines or cytokines. In the current study using proCPR deficient mice, we showed that injection of Con A into the mouse tail vein can induce a significantly higher lethality in proCPR-deficient female but not in male mice. Furthermore, a lack of CPR activity increased serum macrophage inflammatory protein-2 (MIP-2) and high-mobility group box 1 (HMGB1) levels after Con A injection. These in vivo findings suggest that CPR helps to protect against Con A-induced
hepatitis
.
...
PMID:Procarboxypeptidase R deficiency causes increased lethality in concanavalin A-induced hepatitis in female mice. 2060 25
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