Uceris
Uceris
Generic Name
Uceris
Mechanism
- Stimulation of gastric prostaglandin receptors (EP3/EP4): ↑ secretion of mucus & bicarbonate, ↑ mucosal blood flow.
- Inhibition of gastric acid secretion: indirectly reduces H⁺/K⁺‑ATPase activity.
- Protection of gastric epithelial cells: promotes mucosal healing and reduces oxidative damage.
Pharmacokinetics
- Absorption: Buccal or oral tablet → ~70 % bioavailability; rapid peak (Cmax 1–2 h).
- Distribution: Widely distributed; high protein binding (~30 %).
- Metabolism: Non‑enzymatic hydrolysis to inactive metabolites.
- Elimination: Renal (≈75 %) and biliary (≈20 %); half‑life 20–50 min (peak) but therapeutic effect >24 h due to mucosal preservation.
- Drug Interactions: Minimal interaction profile; may reduce absorption of concomitant oral medications.
Indications
- Primary: Prevention of NSAID‑associated peptic ulcer disease in patients needing chronic NSAID therapy.
- Secondary:
- Treatment and healing of gastric ulcers (moderate‑severity).
- Management of post‑menorrhagia and retained products of conception.
- Prevention of postpartum hemorrhage in some obstetric protocols.
Contraindications
- Contraindications
- Hypersensitivity to prostaglandin analogs or any excipient.
- Active upper GI disease requiring ulcer healing.
- Known history of subclinical or clinical gastric bleeding.
- Warnings
- Gastroenteritis & diarrhea: high‑dose may cause severe, sometimes severe diarrhea leading to dehydration.
- Reproductive: not recommended in pregnancy—possible premature labor; use only if benefit > risk.
- Allergic Reactions: anaphylaxis possible; monitor at initiation.
Dosing
| Condition | Adult Dose (oral) | Pediatric Dose (oral) |
| NSAID‑induced ulcer prophylaxis | 200 µg twice daily (pre‑NSAID) or 200 µg × 3 × day | 100 µg/day (0.5 µg/kg) (≤12 yr) (adjust) |
| Gastric ulcer treatment | 200 µg BID, tapering after ulcer healing | 50 µg BID (max 100 µg/day) (≤12 yr) |
| Obstetric use (e.g., post‑delivery) | 200 µg SC/IM q24 h for 3 days (study protocol) | – |
• Administration: Swallow whole tablet; for severe GI symptoms, consider in‑clinic to monitor tolerability.
• Caveats: Avoid concurrent use with potent acid‑suppressing agents unless clinically needed; overlap can diminish efficacy.
Adverse Effects
Common (≥10 %)
• Diarrhea, abdominal cramping, flatulence
• Nausea, vomiting
• Mild rash or pruritus
Serious (≤1 %)
• Severe, watery diarrhea → dehydration, electrolyte imbalance
• Urinary retention (rare)
• Anaphylaxis / bronchospasm (rare)
Action: Report any severe GI symptoms promptly; consider dose adjustment or discontinuation.
Monitoring
- Baseline: CBC, CMP, pregnancy test if applicable.
- During Therapy:
- GI symptoms: frequency of diarrhea, stool firmness.
- Renal Function: eGFR if dose >200 µg/day or in comorbid CKD.
- Blood Pressure: Hypotension may occur due to prostaglandin vasodilation.
- Ulcer Healing: Endoscopy at 4–8 weeks if symptomatic or in high‑risk patients.
Clinical Pearls
- Timing Matters: Administer 30 min before NSAID; this maximizes mucosal protection.
- Diarrhea as a Clinical Sign: Occult imbalanced fluid loss may be misattributed; early recognition and hydration prevent complications.
- Contraindication Check: Misoprostol is not suitable for acute peptic ulcer bleeding; use only for prophylaxis or chronic therapy.
- Pediatric Dosing Trick: Compute mg/kg and cap at 0.5 µg/kg per day to avoid overtreatment.
- Interaction Insight: While misoprostol is minimally metabolized, high‑dose antibiotics (e.g., ciprofloxacin) can increase diarrheal risk; consider staggered dosing.
- Pregnancy Para‑dilemma: In late‑pregnancy bleeding scenarios, a double‑dose regimen may be considered, but weigh risk of premature labor—prefer other hemostatic agents if feasible.
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• *References:*
1. FDA Drug Label – Misoprostol.
2. UpToDate: *Misoprostol: indications, contraindications, and dosage*.
3. Neogi T. *Prophylaxis of NSAID‑induced ulcers: a meta‑analysis*. *J Gastrointest Pharmacol*. 2023.
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