Paradigm shift in treatment of Wilson's disease: zinc therapy now treatment of choice.
Brain Dev. 2006 Apr;28(3):141-6. Epub 2006 Feb 7.
University Department of Neurology, UMC-Utrecht, Heidelberglaan 100, 3584 CX, The Netherlands. tu.hoogenraad@planet.nl
Abstract
Zinc therapy has replaced penicillamine as first-line therapy for Wilson's disease. New guidelines reflect the paradigm shift in treatment that has occurred in recent years. In the old paradigm, Wilson's disease
was seen as genetic disorder associated with the accumulation of copper
in the liver and in other organs once the liver had become overloaded
with copper. When left untreated, the disease was regarded as uniformly fatal. The old treatment
guidelines advised, 'decoppering' with penicillamine because this
chelating agent was considered effective in restoring most patients to
health. Before the start of treatment, patients were warned that their symptoms could worsen during the first weeks or months of therapy, so as to prevent them from abandoning penicillamine therapy in dismay. In the new paradigm, Wilson's disease is seen as a hereditary disorder associated with copper intoxication. The essence of symptomatic Wilson's disease
is poisoning by free copper in the blood, that is, by copper that is
not bound to ceruloplasmin. This form of copper is toxic, whereas
accumulated copper and copper that is bound to ceruloplasmin or
metallothionein is not. The treatment of symptomatic Wilson's disease
is no longer aimed at 'decoppering', the removal of accumulated copper,
but at the normalization of the free copper concentration in blood, to
reverse the copper poisoning. This can be achieved safely and
effectively with zinc therapy. Zinc induces metallothionein, a highly effective detoxification protein that binds copper. Oral zinc therapy leads to storage of metallothionein-bound copper in the mucosa of the gut and to the excretion of copper via the stools. New treatment guidelines advise against the use of chelating agents as initial treatment because they may aggravate copper intoxication and cause iatrogenic deterioration.
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