WILSON’S DISEASE (Hepatolenticular Degeneration)

1. Definition

Wilson’s disease (WD) is an autosomal recessive disorder of copper metabolism due to mutation in the ATP7B gene, leading to:

• ↓ hepatic copper excretion into bile
• ↓ incorporation into ceruloplasmin
• → toxic copper accumulation in:
  • Liver
  • Brain (basal ganglia)
  • Cornea
  • Kidneys

2. Epidemiology

• Age of presentation:
  • Hepatic: childhood (5–15 yrs)
  • Neurological: adolescence/young adults (15–35 yrs)

3. Pathophysiology

Normal copper metabolism

• Absorbed in intestine → transported to liver
• Incorporated into ceruloplasmin via ATP7B
• Excess excreted in bile

In Wilson’s disease

• Defective ATP7B →
  • ↓ biliary excretion
  • ↓ ceruloplasmin binding
• Free copper accumulates → oxidative damage

Target organ injury

• Liver → hepatitis, cirrhosis
• Brain → basal ganglia degeneration
• RBC → hemolysis
• Kidney → tubular dysfunction

4. Clinical Features

A. Hepatic manifestations

• Asymptomatic transaminitis
• Acute hepatitis (mimics viral)
• Chronic hepatitis → cirrhosis
• Acute liver failure (ALF)
  • Coombs-negative hemolysis
  • Low ALP (important clue)
  • ALP:bilirubin ratio < 4

B. Neurological manifestations

• Tremor (classically wing-beating tremor)
• Dysarthria
• Dystonia
• Parkinsonism
• Ataxia

C. Psychiatric features

• Personality changes
• Depression
• Psychosis
• Cognitive decline

D. Ophthalmic signs

• Kayser–Fleischer (KF) rings
  • Copper in Descemet membrane
  • Seen best on slit lamp
  • Almost universal in neuro WD
• Sunflower cataract (rare)

E. Other systemic features

• Hemolytic anemia (Coombs negative)
• Renal tubular dysfunction (Fanconi syndrome)
• Osteopenia
• Cardiomyopathy (rare)

5. Diagnosis 

Leipzig scoring system (gold standard)

• KF rings
• Neurological features
• Ceruloplasmin
• Urinary copper
• Liver copper
• Genetic testing

 Score ≥ 4 = diagnostic

Key investigations

1. Serum ceruloplasmin

• ↓ (< 0.2 g/L)
• BUT:
  • Normal in inflammation/pregnancy
  • Low in malnutrition → false positive

2. 24-hour urinary copper

• 100 µg/day (diagnostic)
• 40 µg/day (suggestive)

3. Hepatic copper concentration

• 250 µg/g dry weight → diagnostic

4. Slit lamp examination

• KF rings

5. Genetic testing

• ATP7B mutation (confirmatory)

6. Blood tests clues (exam pearls)

• Coombs-negative hemolysis
• Low ALP in ALF
• AST > ALT

6. Differential Diagnosis

• Autoimmune hepatitis
• Hemochromatosis
• NAFLD
• Drug-induced liver injury
• Young patient with cirrhosis → always rule out WD

7. Management 

A. General principles

• Lifelong treatment
• Avoid copper-rich foods:
  • Shellfish, nuts, chocolate, mushrooms

B. First-line therapy

1. Chelation therapy

• D-penicillamine
  • First-line (traditional)
  • Increases urinary copper excretion
  • Give with pyridoxine

 Side effects:

• Bone marrow suppression
• Nephrotic syndrome
• Worsening neurological symptoms

• Trientine
  • Better tolerated
  • Preferred if penicillamine intolerant

2. Zinc therapy

• Zinc acetate
  • Blocks intestinal copper absorption
  • Used for:
    • Maintenance
    • Asymptomatic patients

C. Acute liver failure

• Urgent evaluation for transplant

D. Liver transplantation

• Indications:
  • Acute liver failure
  • Decompensated cirrhosis
  • Treatment failure

 Curative (corrects metabolic defect)

8. Monitoring

• Urinary copper
• LFTs
• CBC (for drug toxicity)
• Neurological status

9. Prognosis

• Excellent with early treatment
• Untreated → fatal