Gene/Protein
Disease
Symptom
Drug
Enzyme
Compound
Pivot Concepts:
Gene/Protein
Disease
Symptom
Drug
Enzyme
Compound
Target Concepts:
Gene/Protein
Disease
Symptom
Drug
Enzyme
Compound
Query: UNIPROT:P02774 (
Gc-globulin
)
196
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
Serum
Group-specific component
(a probable vitamin D transport protein) concentrations have been measured in 72 patients with
chronic liver disease
. Low mean values were found in groups of patients with cirrhosis and metastatic liver disease. In a group of patients with biliary tract disease the mean value was not significantly different from normal except for seven patients with severe bone disease who were found to have the lowest levels. The mechanism for the reduction remains to be clarified, but low
Group-specific component
values may play a contributory role in the osteodystrophy of chronic obstructive liver disease.
...
PMID:Group-specific component [Gc] levels in chronic liver disease. 7 53
This doctoral thesis is based on seven previously published papers and reports on the role of the actin-scavenger
Gc-globulin
in acute and chronic liver diseases.
Gc-globulin
is synthesized in the liver and is a multifunctional protein; however, its main physiologic function is presumably actin binding and actin scavenging. Actin is a major cellular protein released during cell necrosis that may cause fatal formation of actin-containing thrombi in the circulation if the actin scavenging capacity of
Gc-globulin
is exceeded. In my studies, I found serum
Gc-globulin
levels to be reduced in liver disease, most so in patients with acute liver failure (ALF). In patients admitted with acetaminophen (paracetamol) overdose,
Gc-globulin
concentrations were lower in patients with hepatic encephalopathy than in those without and the levels nadired at approximately 60-72 hours after acetaminophen ingestion, corresponding with the peak in aminotransferese levels (and thus, hepatic necrosis). In patients with ALF, admission
Gc-globulin
was significantly lower in 47 nonsurvivors than in 30 survivors, 26% and 46% of normal, respectively (P<0.001). The predictive value of outcome using a
Gc-globulin
cutoff level of 100 mg/L equaled that of the internationally accepted King's College Hospital criteria. The prognostic value of
Gc-globulin
was confirmed in a separate study including 106 patients from the United States with nonacetaminophen-induced ALF now using an automated nephelometric assay whereas the prognostic value seemed less obvious for acetaminophen-induced ALF. Multiple organ failure (MOF) is a frequent complication of ALF. In ALF patients with deep coma (hepatic encephalopathy grade III or IV)
Gc-globulin
levels correlated inversely with the number of failing organs. Levels were lower in patients who later developed MOF than in those who did not. Surprisingly, kinetic studies in patients with ALF and acute on
chronic liver disease
showed
Gc-globulin
production to be 7-fold increased in these conditions. Despite this increase
Gc-globulin
levels were severely reduced and the reduction must therefore be due to a highly increased consumption of
Gc-globulin
- probably because of hepatocyte necrosis and removal from the circulation of
Gc-globulin
:actin complexes or because of its role in immune-related functions. Patients with
chronic liver disease
had reduced
Gc-globulin
levels, but the reduction was less pronounced than in ALF. After liver transplantation,
Gc-globulin
concentrations normalized within two weeks, in contrast to the continuous decrease in albumin levels suggesting a very different regulation of these two phylogenetically related proteins. It remains to be studied if lack of
Gc-globulin
contributes to the pathogenesis of patients with ALF or
chronic liver disease
. Future studies should focus on the potential value of
Gc-globulin
substitution in these patients.
...
PMID:Gc-globulin in liver disease. 1923 64
