Wilson disease
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Wilson disease
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Anemia
Wilson disease p. 402
Autosomal recessive disorders
Wilson disease p. 402
Chromosome abnormalities
Wilson disease p. 402
Cirrhosis p. 396
Wilson disease p. 402
Copper metabolism
Wilson disease p. 402
Fanconi syndrome p. 604
Wilson disease p. 402
Hemolytic anemia p. 427
Wilson disease p. 402
Hepatitis
Wilson disease p. 402
Kayser-Fleischer rings
Wilson disease as cause p. 402
Liver failure
Wilson disease as cause p. 402
Parkinsonism
Wilson disease as cause p. 402
Penicillamine
for Wilson disease p. 402
Renal disease
Wilson disease p. 402
Wilson disease p. 402
chromosome association p. 62
Fanconi syndrome p. 604
free radical injury and p. 211
Zinc p. 69
Wilson disease p. 402
Transcript
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One essential mineral that our body needs to get through the diet is copper, and typically we take in about 1 to 2 mg per day from the food we eat, things like whole grains, beans, nuts and potatoes; but really our body only needs about 0.75 mg / day, so that extra copper is excreted.
About 90% of the excess copper is excreted into the bile, where it eventually ends up as fecal copper, and the other 10% is excreted in the urine.
In Wilson disease, there’s genetic defect that results in the excess copper being kept in the body and deposited in various tissues...where it’s not supposed to be, and just like iron, free copper reacts with hydrogen peroxide in the body to form the hydroxyl radical, a reactive oxygen species that’s pretty good at damaging tissue, so over time those tissues are seriously damaged by free radical generation.
Now your liver cells, or hepatocytes, play a really important role in helping the body get rid of excess copper.
So usually the copper from the diet is absorbed in the small intestine via enterocytes, and passed off into the portal vein to the liver.
Once it’s in the liver it’s sent to a special transport protein called ATP7B, which has a couple super important jobs.
The first job, is that it binds copper to apoceruloplasmin, which is the major copper-carrying protein in the blood and is responsible for carrying 95% of the copper in blood.
After it binds copper it’s then just called ceruloplasmin, and this guy can haul 6 molecules of copper at once.
ATP7B’s other job is to gather up the rest of the copper into vesicles to be exocytosed into into the bile canaliculi, where it goes into the bile and is eventually excreted.
With Wilson disease, there’s an autosomal recessive defect in this ATP7B transport protein. As you could probably guess, that means it can’t incorporate the copper into ceruloplasmin or excrete it into the bile.
Since it’s not doing either of these things anymore, the copper builds up inside the hepatocyte and starts to produce free radicals.
Eventually, all this built up copper and free-radical damage injures or destroys the hepatocyte, causing free copper to spill out into the interstitial space and from there into the blood supply, where it’s circulated to and deposited in other tissues, where it also causes free radical damage over time.
Resumen
Wilson disease is a rare autosomal recessive genetic disorder that causes excessive accumulation of copper in various tissues of the body, particularly the liver, and brain as a result of a mutation in the ATP7B gene. Symptoms of Wilson disease can vary widely and may include fatigue, abdominal pain, muscle stiffness or tremors, and a characteristic brown ring around the cornea of the eye known as a Kayser-Fleischer ring. Over time, copper accumulation in the liver can lead to liver disease and cirrhosis, and copper accumulation in the brain can cause neurological symptoms such as movement disorders, psychiatric symptoms, and cognitive decline.
Fuentes
- "Robbins Basic Pathology" Elsevier (2017)
- "Harrison's Principles of Internal Medicine, Twentieth Edition (Vol.1 & Vol.2)" McGraw-Hill Education / Medical (2018)
- "Pathophysiology of Disease: An Introduction to Clinical Medicine 8E" McGraw-Hill Education / Medical (2018)
- "CURRENT Medical Diagnosis and Treatment 2020" McGraw-Hill Education / Medical (2019)
- "Molecular pathogenesis of Wilson and Menkes disease: correlation of mutations with molecular defects and disease phenotypes" Journal of Medical Genetics (2007)
- "Molecular pathogenesis of Wilson and Menkes disease: correlation of mutations with molecular defects and disease phenotypes" Journal of Medical Genetics (2007)
- "A practice guideline on Wilson disease" Hepatology (2003)