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Treatment of Wilson disease Treatment of Wilson disease Valentina Medici, M.D. Division of Gastroenterology and Hepatology UC Davis May 2 nd , 2009

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Treatment of Wilson diseaseTreatment of Wilson disease

Valentina Medici, M.D.Division of Gastroenterology and Hepatology

UC DavisMay 2nd, 2009

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OutlineOutline

• Treatment options• Mechanism of action• Side effects• Strategies for better management• New prospectives

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OptionsOptions

• Chelating agents (Penicillamine, Trientine)• Zinc• Tetrathiomolybdate (?)

• Diet • Liver Transplantation

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intestine

Copper

CeruloplasminPenicillamine/Trientine

urine

Chelating Chelating agentsagents: Penicillamine : Penicillamine and Trientineand Trientine

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PenicillaminePenicillamine

• Copper chelator: ↑ Cu urinary excretion• Dose: 750-1500 mg/daily + pyridoxine (B6)

daily• 30% discontinued for side effects• Can worsen neurological symptoms (up to 50%)• Rare birth defects (“cutis laxa”)

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Penicillamine Penicillamine side effectsside effects

• Fever, rash, lymphoadenopathy• Aplastic anemia, neutropenia and

thrombocytopenia• Late side effects: elastosis perforans serpiginosa,

arthropathy, lupus-like reaction, nephrotic syndrome, myastenia gravis, Goodpasture syndrome

Scheinberg IH, Sternlieb I. Wilson’s disease. In: Smith LH Jr., Ed. Philadelphia: W.B. Saunders, 23;1984

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TrientineTrientine

• Cu chelator• New “first choice”• Fewer side effects than penicillamine• More tolerable for neurological symptoms• Dose: 750 -1500 mg/daily• Side effects rare pancytopenia

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Zinc Sulfate/AcetateZinc Sulfate/Acetate

“Blocks” Cu absorption• Prevents Cu toxicity∀↓ Cu Urinary Excretion• Minor side effects (dyspepsia): Acetate is better tolerated• Dose: 150 mg daily of elemental zinc• Slow action (4-6 months)• No concerns during pregnancy, safe for neurological

symptoms

Brewer GJ, J Lab Clin Med, 1999

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Combination therapyCombination therapy

• Penicillamine + Zinc dubious efficacy

• Trientine + Zinc yes for decompensated cirrhosis

Askari, JLabClinMed, 2003

Brewer, JAmCollNutr, 1993

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TetrathiomolybdateTetrathiomolybdate

• Forms a complex with copper and protein• Taken with meals complexes Cu in the

food and is secreted into the intestine; between meals it is absorbed and complexes Cu in the blood with albumin

• More efficacy for neurological symptoms• Not yet approved

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• 23 pts on Trientine• 25 pts on TM8 weeksTrientine26% risk of

neuro deteriorationTM 4% risk of neuro

deterioration

Tetrathiomolybdate (TM) for Tetrathiomolybdate (TM) for neurological symptomsneurological symptoms

Brewer GJ, Arch Neurol, 2006

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0

1000

2000

3000

4000

5000

6000

7000

8000

basal 1 2 3 4 5 6 7 9 11 13

weeks

ug/2

4 h

0

200

400

600

800

1000

1200

1400

U/L

24h-urine copper

24h-urine zinc

serum ALT

Medici V, Mov Disord, 2006

33 yo, man, with severe neurological WD33 yo, man, with severe neurological WD

TTM TTM 120 mg/day120 mg/day

TTM TTM 180 mg/day180 mg/day

stop TTMstop TTM

150327486642171Chol

358338346299221Alk phos

87842120734985ALT

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IndicationsIndications

Hepatic disease (or first choice?)

Neurological disease

Penicillamine side effects

TrientineTrientine

Neurological patients?Tetrathiomolybdate?Tetrathiomolybdate?

Neurological disease

Maintenance treatment

Pregnancy

ZincZinc

Hepatic diseasePenicillaminePenicillamine

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Management during follow upManagement during follow up

• Depends on the severity of the neurological or hepatic features

• Assess any sign of hepatic decompensation

• 24-h urinary Cu excretion (denotes adequate treatment)

• Monitor penicillamine side effects

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Management of hepatic WDManagement of hepatic WD

• About 30% of patients have mildly increased transaminase level benign

• Liver biopsy• Try an alternative anti-copper agent• Add Vitamin E (antioxidant effect)

von Herbay A, J Hepatol, 1994

Iorio, J Pediatr Gastroenterol Nutr, 2004

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ComplianceCompliance

Sudden interruption of therapy in Wilson

disease can result in Acute Liver Failure

Walshe, Lancet, 1986

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Gene therapyGene therapy

Lentiviral gene Lentiviral gene transfer (ATP7B)transfer (ATP7B)

Increased levels of ceruloplasmin

Reduced hepatic copper

Improved hepatic fibrosis

Merle, Scand J Gastro, 2006

LEC ratsLEC rats

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Allen KJ, Cell Transplant, 2004

TOXIC MILK MOUSE

(N° 46)

Sublethal radiation

Transplant with bone marrow

stem cells

N°11 (24%): liver ripopulation + Reduction of

hepatic copper accumulation

Bone marrow stem cellsBone marrow stem cells

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Hepatocytes transplantationHepatocytes transplantation

Joseph, Gastro, 2009

Spleen

LiverHepatocytes

LEC rats

• 6 months after transplant: liver was extensively repopulated with hepatocytes

• ATP7B expression, increased Cp, reduced hepatic Cu

• Improved liver histology

Cholic acid, radiation, partial hepatectomy

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ConclusionsConclusions• WD is a very peculiar medical situation genetic

but treatable disorder, almost complete resolution of symptoms with appropriate and timely therapy

• Early diagnosis and early therapy are mandatory

• Compliance to medical treatment is crucial