Uribel
Ursodeoxycholic acid
Generic Name
Ursodeoxycholic acid
Mechanism
- Reduces cholesterol solubility in bile by replacing toxic bile acids with the hydrophilic ursodeoxycholic acid.
- Inhibits cholesterol micelle formation → ↓ nucleation & aggregation of cholesterol crystals.
- Stimulates bile flow and protects hepatocyte membranes from bile acid toxicity.
- Promotes enterohepatic circulation, allowing repeated use of the drug within the intestine.
Pharmacokinetics
- Absorption: 30–65 % orally; 20 % higher when taken with food.
- Bioavailability: ~50 % due to hepatic first‑pass glucuronidation.
- Metabolism: conjugated (glucuronide, sulfate) primarily in the liver.
- Excretion: 90 % into bile, 10 % renal; hepatic transporters (OATP1B1/3) are critical.
- Half‑life: 8–10 h; terminal phase prolonged by enterohepatic recycling.
Indications
- Cholesterol gallstone dissolution (selected patients with < 3 cm stones).
- Prevention of gallstone recurrence after cholecystectomy.
- Primary biliary cholangitis (as adjunct in cholestasis).
- Bariatric‑surgery prophylaxis (to reduce post‑operative gallstone risk).
- Idiopathic cholestatic liver disease (infants or adults).
- Conservative management of mild gallstone pancreatitis (small impacted stones).
Contraindications
- Choledocholithiasis / biliary obstruction (unless surgery planned).
- Known hypersensitivity to ursodeoxycholic acid or excipients.
- Severe hepatic impairment—use cautiously; limit dose.
- Pregnancy: Category B; use only if benefits > risks.
- Breastfeeding: excreted in milk; counsel patient.
Dosing
| Population | Dose | Frequency | Notes |
| Adults (gallstone dissolution) | 1–2 g/day | Divided doses (e.g., 200 mg q6h) | Start at 300–600 mg/day for tolerance, then titrate. |
| Adults (prevention post‑cholecystectomy) | 600 mg/day | Divided | Continue 12 mo. |
| Pediatrics | 10–12 mg/kg/day | Divided | Weight‑adjusted; monitor growth. |
• Take with meals to enhance absorption.
• Monitor LFTs; if ALP < 1.5 × ULN after 6 mo, consider dose reduction.
Adverse Effects
| Severity | Adverse Effect | Incidence |
| Common (≤10 %) | Nausea, diarrhea, flatulence, headache | Up to 10 % |
| Common | Mild pruritus | ≤5 % |
| Serious (≤1 %) | Cholestatic hepatitis (↑AST/ALT, ALP) | <1 % |
| Serious | Severe allergic reaction (rash, anaphylaxis) | <0.5 % |
| Rare | Myopathy (especially with statins) | <0.1 % |
Management: Discontinue immediately if signs of hepatic injury (jaundice, markedly ↑LFTs).
Monitoring
- Baseline + every 4–6 weeks: AST, ALT, ALP, total bilirubin.
- Renal function: Cr/ BUN if renal disease present.
- Ultrasound: baseline, then every 6–12 mo (stone dissolution or recurrence).
- Symptom diary: GI upset, pruritus, rash.
Clinical Pearls
- Combination therapy: Adding *ezetimibe* reduces hepatic cholesterol production, accelerating stone dissolution.
- Dose splitting: Taking divided doses around meals maximizes enterohepatic cycling and efficacy.
- Titration guard rails: Begin at 300–600 mg/day to reduce GI intolerance, then increase to 1–2 g/day only after tolerance.
- Myopathy vigilance: Do not co‑administer with statins unless patients are under close monitoring or the statin has a lower myopathy risk profile.
- Prophylaxis advantage: A 12‑month regimen after cholecystectomy lowers gallstone recurrence by ~45 % in high‑risk groups (e.g., patients with hyperlipidemia or rapid weight loss).
- Pregnancy safety: Though Category B, if the patient becomes pregnant during therapy, consider continuing only if clinically warranted and discuss risks.
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• Key pharmacology terms: *ursodeoxycholic acid, bile acid therapy, cholesterol gallstones, hepatobiliary, enterohepatic circulation, cholestasis*.