Generic Name

Esomeprazole

Mechanism

• Target: The *gastric H⁺/K⁺‑ATPase* (proton pump) located on parietal cells.
• Binding: Esomeprazole’s sulfenamide moiety covalently attaches to *cysteine* residues (Cys292/Cys344) on the enzyme, leading to irreversible inhibition.
• Kinetics: Inhibits 70–80 % of the pump at therapeutic concentrations; maximal effect occurs 1–2 hrs after dosing.
• Result: Sustained inhibition of acid secretion for 24 hrs with each dose, even in the presence of pepsinogen‑stimulated secretion.

Pharmacokinetics

Indications

• Gastro‑oesophageal reflux disease (GERD): erosive esophagitis, non‑erosive reflux disease (NERD).
• Peptic ulcer disease: healing and maintenance of ulcers (gastric, duodenal, NSAID‑related).
• Helicobacter pylori eradication: in triple or quadruple therapy regimens.
• Zollinger–Ellison syndrome: control of hyper‑secretory gastrinomas.
• Pre‑operative acid suppression: reduce aspiration risk in elective surgeries.

Contraindications

• Contraindications: Hypersensitivity to esomeprazole or other PPIs.
• Warnings:
• *Long‑term use* (>12 mo): ↑ risk of *osteoporosis*, *Clostridioides difficile* colitis, *electrolyte disturbances* (hypomagnesemia).
• *Pregnancy*: Category B – limited human data; use only if benefits outweigh risks.
• *Pediatric*: <12 yrs – use with caution; data are limited.
• *Renal impairment*: dose adjustments not required; monitor for signs of hepatic dysfunction.

Dosing

• Capsules or tablets; chewable forms available for gastro‑retentive delivery.
• For IV: 40 mg over 30 min, then 20 mg q12h for 1–3 days.
• *Switching* from other PPIs: give esomeprazole 1 day before next dose to maintain acid suppression.

Adverse Effects

• Common (≤10%)
• Headache, abdominal pain, flatulence, constipation, diarrhoea, nausea, dyspepsia.
• Serious
• *Clostridioides difficile* colitis, electrolyte disturbances (hypomagnesemia), *severe* cutaneous reactions (SJS/TEN).
• *Cardiovascular*: rare reports of QT prolongation.
• *Renal*: interstitial nephritis, acute tubular necrosis (rare).

Monitoring

• Baseline: CBC, CMP, ESR/CRP, Vit‑B12 (long‑term use).
• Periodic:
• Serum magnesium (every 3–6 mo).
• Bone density scan (if >5 yrs therapy).
• Renal function (if at risk).
• Follow‑up: Symptom resolution; endoscopy for GERD/ulcer after 4 weeks of therapy.

Clinical Pearls

• First‑bite advantage: Esomeprazole (the S‑enantiomer of omeprazole) exhibits higher plasma concentrations and longer acid‑inhibition duration compared with its racemate.
• Rapid onset: Absorbed quickly; peak plasma levels are reached in ~1 hr—ideal for acute reflux episodes.
• CYP2C19 genotype matters: *Poor metabolizers* achieve 2–3× higher drug exposure → consider lower doses or monitor for toxicity.
• Avoid PPIs with antacids: Antacids raise gastric pH, reducing esomeprazole absorption; if needed, separate administration by ≥1 hr.
• Switching pitfalls: Transitioning from a strong CYP inhibitor (e.g., ketoconazole) to esomeprazole can cause drug accumulation → dose‐adjust if needed.
• Post‑operative prophylaxis: A single 20 mg dose pre‑induction significantly reduces gastric acid‑related aspiration events in high‑risk patients.

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• *For detailed references, consult the latest clinical guidelines and peer‑reviewed pharmacology texts (e.g., "Goodman & Gilman's The Pharmacological Basis of Therapeutics," UpToDate.*