New insights into the pathogenesis of copper toxicosis in Wilson's disease: evidence for copper incorporation and defective canalicular transport of caeruloplasmin

Previous studies have suggested that copper is incompletely incorporated into caeruloplasmin, the major plasma form of copper-transporting protein, in the genetic copper toxic condition, Wilson's disease. In this paper we have investigated the role of copper and caeruloplasmin in the abnormal b...

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Bibliographic Details
Published in:Biochemical journal 1996-05, Vol.315 (3), p.851-855
Main Authors: Chowrimootoo, G.F.E, Ahmed, H.A, Seymour, C.A
Format: Article
Language:English
Subjects:
Apoproteins - metabolism
bile
Bile - metabolism
biliary canalicular membranes
biliary copper excretion
biliary tract
Biliary Tract - metabolism
Biliary Tract - ultrastructure
binding proteins
biomarkers
Carrier Proteins - metabolism
Ceruloplasmin - metabolism
copper
Copper - adverse effects
Copper - metabolism
enzymes
excretion
ferroxidase
hepatocytes
hepatolenticular degeneration
Hepatolenticular Degeneration - etiology
Hepatolenticular Degeneration - metabolism
Homeostasis
Humans
hydrolases
In Vitro Techniques
Ion Transport
Liver - metabolism
markers
Microscopy, Electron
nutrient transport
oxidoreductases
patients
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Summary:Previous studies have suggested that copper is incompletely incorporated into caeruloplasmin, the major plasma form of copper-transporting protein, in the genetic copper toxic condition, Wilson's disease. In this paper we have investigated the role of copper and caeruloplasmin in the abnormal biliary copper transport that characterizes Wilson's disease. Using SDS/PAGE and Western blotting, we have demonstrated the presence of holocaeruloplasmin in liver samples from patients with Wilson's disease (abnormal biliary copper excretion) and in control patients (normal biliary copper excretion). The presence of holocaeruloplasmin was also confirmed by measurement of caeruloplasmin oxidase activity using staining with o'Dianisidine. In contrast with the findings in liver tissue, holocaeruloplasmin was absent from bile from patients with Wilson's disease, but as expected it was present in the bile from control subjects. We have also identified and partially characterized a 189-200 kDa protein from purified human biliary canalicular membranes which binds copper and possesses caeruloplasmin-like activity when probed with a specific human anti-caeruloplasmin antibody. In conclusion, we have demonstrated that copper incorporation in caeruloplasmin is normal in patients with Wilson's disease contrary to previous reports. Secondly, we have shown that the defect in Wilson's disease appears to lie in the biliary canalicular excretion of holocaeruloplasmin resulting in its retention within the hepatocyte causing copper toxicosis. Finally we have identified and partially characterized a caeruloplasmin-binding protein from biliary canalicular membranes which may provide a link to the gene defect in Wilson's disease.
ISSN:0264-6021
1470-8728
DOI:10.1042/bj3150851