Aberrant expression of copper associated genes after copper accumulation in COMMD1-deficient dogs

COMMD1-deficient dogs progressively develop copper-induced chronic hepatitis. Since high copper leads to oxidative damage, we measured copper metabolism and oxidative stress related gene products during development of the disease. Five COMMD1-deficient dogs were studied from 6 months of age over a p...

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Published in:Journal of trace elements in medicine and biology 2015-01, Vol.29, p.347-353
Main Authors: Favier, Robert P., Spee, Bart, Fieten, Hille, van den Ingh, Ted S.G.A.M., Schotanus, Baukje A., Brinkhof, Bas, Rothuizen, Jan, Penning, Louis C.
Format: Article
Language:English
Subjects:
Adaptor Proteins, Signal Transducing - deficiency
Adaptor Proteins, Signal Transducing - metabolism
Alanine Transaminase - blood
Animals
Bile Acids and Salts - metabolism
Cation Transport Proteins - genetics
Cation Transport Proteins - metabolism
COMMD1-deficient dogs
Copper - metabolism
Copper accumulation
Dogs
Female
Gene Expression Profiling
Gene Expression Regulation
Hepatitis - blood
Hepatitis - pathology
Male
Translational research
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Summary:COMMD1-deficient dogs progressively develop copper-induced chronic hepatitis. Since high copper leads to oxidative damage, we measured copper metabolism and oxidative stress related gene products during development of the disease. Five COMMD1-deficient dogs were studied from 6 months of age over a period of five years. Every 6 months blood was analysed and liver biopsies were taken for routine histological evaluation (grading of hepatitis), rubeanic acid copper staining and quantitative copper analysis. Expression of genes involved in copper metabolism (COX17, CCS, ATOX1, MT1A, CP, ATP7A, ATP7B, ) and oxidative stress (SOD1, catalase, GPX1 ) was measured by qPCR. Due to a sudden death of two animals, the remaining three dogs were treated with d-penicillamine from 43 months of age till the end of the study. Presented data for time points 48, 54, and 60 months was descriptive only. A progressive trend from slight to marked hepatitis was observed at histology, which was clearly preceded by an increase in semi-quantitative copper levels starting at 12 months until 42 months of age. During the progression of hepatitis most gene products measured were transiently increased. Most prominent was the rapid increase in the copper binding gene product MT1A mRNA levels. This was followed by a transient increase in ATP7A and ATP7B mRNA levels. In the sequence of events, copper accumulation induced progressive hepatitis followed by a transient increase in gene products associated with intracellular copper trafficking and temporal activation of anti-oxidative stress mechanisms.
ISSN:0946-672X
1878-3252
DOI:10.1016/j.jtemb.2014.06.007