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Drug Monograph

Nexium (Esomeprazole)

esomeprazole magnesium

Proton Pump Inhibitor (PPI) — S-enantiomer of omeprazole·Oral / IV
Pharmacokinetic Profile
Half-Life
1–1.5 h (effect lasts ≥24 h)
Metabolism
CYP2C19 (primary), CYP3A4
Protein Binding
97%
Bioavailability
64% (single 40 mg); ~90% (steady-state 40 mg)
Volume of Distribution
16–18 L
Clinical Information
Drug Class
Proton Pump Inhibitor (substituted benzimidazole; S-isomer)
Available Doses
20, 40 mg capsules; 2.5, 5, 10, 20, 40 mg suspension packets; 20, 40 mg IV vials; 24.65 mg OTC capsule
Route
Oral / Intravenous
Renal Adjustment
None required
Hepatic Adjustment
Child-Pugh C: max 20 mg QD (EE/NSAID/H.pylori); start 20 mg BID (ZE)
Pregnancy
Available data have not demonstrated increased risk of major birth defects
Lactation
Omeprazole (racemate) detected in breast milk; caution advised
Schedule
Rx and OTC (20 mg delayed-release capsule)
Generic Available
Yes (widely)
Pharmacogenomic Note
CYP2C19 PM: ~2-fold higher AUC (less variable than omeprazole)
Rx

Indications

IndicationApproved PopulationTherapy TypeStatus
Healing of erosive esophagitis (EE)Adults + pediatrics ≥1 monthMonotherapyFDA Approved
Maintenance of healing of EEAdultsMonotherapyFDA Approved
Symptomatic GERDAdults + pediatrics ≥1 yearMonotherapyFDA Approved
Risk reduction of NSAID-associated gastric ulcerAdults ≥60 yrs and/or history of gastric ulcerMonotherapyFDA Approved
H. pylori eradication (to reduce duodenal ulcer recurrence)AdultsTriple therapy (+ amoxicillin + clarithromycin)FDA Approved
Pathological hypersecretory conditions (Zollinger-Ellison syndrome)AdultsMonotherapyFDA Approved

Esomeprazole is the S-enantiomer of omeprazole, approved in the United States in 2001. Compared with racemic omeprazole, esomeprazole undergoes less first-pass hepatic metabolism via CYP2C19, resulting in higher and more consistent systemic bioavailability. This translates to somewhat greater and more predictable acid suppression across the population, including CYP2C19 extensive metabolizers. A notable advantage over omeprazole is the specific FDA-approved indication for NSAID-associated gastric ulcer risk reduction in at-risk adults. Esomeprazole is available by prescription and over-the-counter (20 mg).

Off-Label Uses

Stress ulcer prophylaxis (ICU): Widely used in critically ill patients; supported by guideline recommendations in those with GI bleeding risk factors. Evidence quality: Moderate.

NSAID-induced gastric ulcer healing (active ulcer): While the FDA indication covers risk reduction (prevention), esomeprazole is also used off-label to heal established NSAID-induced ulcers, with clinical trial support. Evidence quality: High.

Functional dyspepsia: Empiric PPI trial recommended by ACG/CAG guidelines as initial management. Evidence quality: Moderate.

Dose

Dosing

Adult Dosing — By Clinical Scenario

Clinical ScenarioStarting DoseMaintenance DoseMaximum DoseNotes
Healing of erosive esophagitis20 or 40 mg QD20 or 40 mg QD40 mg/day4 to 8 weeks; if not healed, additional 4 to 8 weeks may be considered
Child-Pugh C: max 20 mg QD
Maintenance of healing of EE20 mg QD20 mg QD20 mg/dayControlled studies did not extend beyond 6 months
Symptomatic GERD (adults)20 mg QD20 mg QD20 mg/day4 weeks; if symptoms unresolved, additional 4 weeks may be considered
OTC: 20 mg QD x 14 days; may repeat every 4 months
NSAID-associated gastric ulcer risk reduction20 or 40 mg QD20 or 40 mg QD40 mg/dayUp to 6 months; 40 mg did not show additional benefit over 20 mg in clinical trials
For patients ≥60 yrs and/or with gastric ulcer history; Child-Pugh C: max 20 mg QD
H. pylori eradication — triple therapy40 mg QD + amoxicillin 1000 mg BID + clarithromycin 500 mg BID40 mg/day10 days
Child-Pugh C: max 20 mg QD; if clarithromycin resistance suspected, consider alternative regimen per ACG guidelines
Zollinger-Ellison syndrome / pathological hypersecretion40 mg BIDIndividualized240 mg/dayTitrate to acid output; some patients require divided doses >80 mg/day
Child-Pugh C: start 20 mg BID

Pediatric Dosing

Indication / AgeDoseDurationNotes
Symptomatic GERD (12–17 yrs)20 mg QD4 weeksCapsules or oral suspension
Symptomatic GERD (1–11 yrs)10 mg QDUp to 8 weeksOral suspension only for this age group
EE healing (12–17 yrs)20 or 40 mg QD4–8 weeksSame dose range as adults
EE healing (1–11 yrs, <20 kg)10 mg QD8 weeksOral suspension; weight-based per PI
EE healing (1–11 yrs, ≥20 kg)10 or 20 mg QD8 weeksOral suspension; weight-based per PI
EE due to acid-mediated GERD (1 month–<1 yr)Weight-based per PIUp to 6 weeksOral suspension only; safety and efficacy for symptomatic GERD not established in <1 yr
Clinical Pearl: Esomeprazole vs Omeprazole

The key pharmacokinetic advantage of esomeprazole over racemic omeprazole is its reduced susceptibility to CYP2C19-mediated first-pass metabolism. This results in approximately 90% bioavailability at steady state (40 mg) compared with approximately 60% for omeprazole. Consequently, CYP2C19 genotype has a smaller impact on esomeprazole exposure: poor metabolizers show only a 2-fold higher AUC with esomeprazole versus a 5–10-fold higher AUC with omeprazole. In clinical practice, this means more predictable acid suppression across genetically diverse populations. However, head-to-head trials have shown only modest clinical differences in EE healing rates, and many guidelines consider PPIs within the class to be broadly interchangeable for most indications.

PK

Pharmacology

Mechanism of Action

Esomeprazole is the S-enantiomer of omeprazole, a substituted benzimidazole proton pump inhibitor. Like all PPIs, it is a prodrug that concentrates in the acidic secretory canaliculi of gastric parietal cells, where the low pH environment converts it to a sulfenamide that forms an irreversible covalent disulfide bond with cysteine residues on the H+/K+-ATPase (proton pump). This covalent inactivation of the final step of gastric acid secretion provides acid suppression that far outlasts the drug’s plasma half-life, persisting for 24 hours or longer until new pump molecules are synthesized. After 5 days of daily dosing with 40 mg, the percentage of time with intragastric pH above 4 exceeds 68% over a 24-hour period.

ADME Profile

ParameterValueClinical Implication
AbsorptionEnteric-coated granules; bioavailability ~64% (single 40 mg dose) rising to ~90% at steady state; Tmax ~1.5 h; AUC decreased 43–53% when taken after eatingHigher and more consistent bioavailability than racemic omeprazole due to reduced CYP2C19-mediated first-pass metabolism of the S-isomer; must take ≥1 hour before meals for optimal absorption
DistributionVd 16–18 L; 97% protein bound; concentrates in parietal cell canaliculi via acid-trappingProtein binding limits dialysis utility; target-site concentration exceeds plasma levels due to ion trapping in acidic canaliculi
MetabolismHepatic via CYP2C19 (primary; forms 5-hydroxy metabolite) and CYP3A4 (forms sulfone metabolite); CYP2C19 PM have ~2-fold higher AUC at steady state; S-isomer is relatively resistant to CYP2C19 metabolism compared with R-omeprazoleCYP2C19 polymorphism has less impact on esomeprazole than omeprazole (2-fold vs 5–10-fold AUC difference in PM); CYP2C19 inhibition underlies clopidogrel interaction; AUC increases non-linearly above 40 mg
Eliminationt1/2 ~1–1.5 h; ~80% excreted in urine as metabolites; <1% unchanged in urine; remainder in fecesDespite short half-life, irreversible pump inactivation provides ≥24 h acid suppression; severe hepatic impairment (Child-Pugh C) substantially increases exposure — dose reduction required
SE

Side Effects

1–10%Common (from clinical trials)
Adverse EffectIncidenceClinical Note
Headache2–11%Most commonly reported; incidence varies by population and formulation; 8% in adolescents 12–17 yrs
Diarrhea2–4%If persistent or severe, consider C. difficile testing
Abdominal pain1–6%Evaluate for underlying pathology if persistent; 3% in adolescents
Nausea1–6%Higher incidence with IV formulation (6%); generally transient with oral forms
Flatulence1–10%Higher incidence with IV formulation (10%); ~1% with oral; related to altered gut flora
Constipation≥1%Manage with fiber and hydration
Dry mouth1–4%Higher with IV formulation (4%)
Dizziness≤3%More common with IV formulation; generally self-limiting
Somnolence2% (children 1–11 yrs)Pediatric-specific finding; not reported at similar rates in adults
SeriousSerious (Regardless of Frequency)
Adverse EffectEstimated FrequencyTypical OnsetRequired Action
C. difficile-associated diarrheaUncommon; risk increases with durationAny time during or after therapyTest stool for C. difficile; discontinue PPI if confirmed; initiate directed antibiotic therapy
HypomagnesemiaRare; mainly with >1 year useMonths to yearsCheck serum magnesium if symptoms (tetany, arrhythmia, seizures); supplement and consider PPI discontinuation; may lead to secondary hypocalcemia and hypokalemia
Bone fractures (hip, wrist, spine)Observational data; risk with long-term high-dose useLong-term (≥1 year)Use lowest effective dose; ensure adequate calcium and vitamin D; FDA class-wide warning
Severe cutaneous adverse reactions (SJS, TEN, DRESS, AGEP)Very rare (postmarketing)Days to weeksDiscontinue immediately at first signs; can be fatal if untreated
Acute interstitial nephritisRare (postmarketing)Weeks to monthsMonitor renal function; discontinue PPI
Cutaneous or systemic lupus erythematosusRare (postmarketing)Weeks to yearsDiscontinue PPI; most CLE cases resolve; evaluate for systemic involvement
Vitamin B12 deficiencyRare; with >3 years useYearsScreen B12 in long-term patients; supplement if deficient
Fundic gland polypsRisk increases with >1 year useMonths to yearsGenerally benign and reversible; use shortest PPI duration necessary
Hypersensitivity (anaphylaxis, angioedema)Rare (postmarketing)Any timeDiscontinue permanently; contraindicated in benzimidazole hypersensitivity
DiscontinuationDiscontinuation Considerations
Short-Term Use (≤8 weeks)
Well tolerated
Generally no rebound symptoms; discontinuation rates in clinical trials comparable to placebo
Long-Term Discontinuation
Rebound acid hypersecretion
After ≥8 weeks of daily use, abrupt stopping may cause rebound heartburn for 1–2 weeks; consider tapering or step-down to H2RA
Long-Term PPI Safety

The long-term safety profile of esomeprazole is shared across the PPI class. Reassess the need for continued therapy after the initial treatment course (4–8 weeks for uncomplicated GERD). Continuous long-term use is appropriate for Barrett esophagus, severe EE (LA Grade C/D), documented bleeding ulcer history, ZE syndrome, and chronic NSAID co-therapy in high-risk patients. For all others, use the lowest effective dose for the shortest duration, with periodic deprescribing assessments.

Int

Drug Interactions

Esomeprazole shares the same drug interaction profile as racemic omeprazole. It inhibits CYP2C19 (affecting clopidogrel activation and metabolism of CYP2C19 substrates) and elevates gastric pH (impairing absorption of pH-dependent drugs). Esomeprazole is itself metabolized by CYP2C19 and CYP3A4, making it susceptible to strong inducers of these enzymes.

MajorClopidogrel
MechanismCYP2C19 inhibition impairs conversion of clopidogrel prodrug to active metabolite
EffectReduced antiplatelet activity; manufacturer of clopidogrel recommends avoidance of both omeprazole and esomeprazole
ManagementAVOID; consider pantoprazole (weaker CYP2C19 inhibition) or H2RA if acid suppression needed
FDA PI
MajorRilpivirine
MechanismElevated gastric pH markedly reduces rilpivirine absorption
EffectLoss of virologic suppression; risk of HIV resistance
ManagementCONTRAINDICATED
FDA PI
MajorHigh-Dose Methotrexate
MechanismPPIs may delay renal elimination of methotrexate
EffectElevated methotrexate and metabolite levels; toxicity risk
ManagementConsider temporary PPI discontinuation; monitor methotrexate levels
FDA PI
ModerateSt. John’s Wort / Rifampin
MechanismCYP2C19 and CYP3A4 induction substantially reduces esomeprazole levels
EffectReduced acid suppression; treatment failure
ManagementAVOID concomitant use
FDA PI
ModerateTacrolimus
MechanismCYP2C19/CYP3A4 inhibition may increase tacrolimus levels
EffectPotential for tacrolimus toxicity
ManagementMonitor tacrolimus trough levels when initiating, adjusting, or stopping esomeprazole
FDA PI
ModerateDiazepam / Phenytoin / Cilostazol
MechanismCYP2C19 inhibition delays clearance of these substrates; 45% reduction in diazepam clearance observed
EffectIncreased exposure to co-administered CYP2C19 substrates
ManagementMonitor phenytoin levels; reduce cilostazol dose; use caution with diazepam
FDA PI
MinorKetoconazole / Iron / Atazanavir / Mycophenolate (pH-dependent absorption)
MechanismElevated gastric pH reduces dissolution and absorption of pH-dependent drugs
EffectDecreased bioavailability of the affected drugs
ManagementMonitor efficacy; separate dosing where possible; for MMF, use the enteric-coated formulation (mycophenolate sodium)
FDA PI
MinorDigoxin
MechanismElevated gastric pH increases digoxin absorption by ~10%
EffectModest increase in digoxin levels; up to 30% in some individuals
ManagementMonitor digoxin levels in patients on narrow therapeutic ranges
FDA PI
Mon

Monitoring

  • Symptom Response4–8 weeks
    Routine    Reassess need for continued PPI. If no erosive disease or high-risk features, consider step-down, on-demand dosing, or H2RA switch. Do not continue indefinitely without clinical indication.
  • Serum MagnesiumPeriodically in long-term use
    Trigger-based    Hypomagnesemia reported with ≥3 months PPI use (most cases >1 year). Check if symptoms suggest deficiency (tetany, tremor, arrhythmias). Consider monitoring calcium in those at risk of hypocalcemia.
  • Vitamin B12Periodically if >3 years use
    Trigger-based    Chronic acid suppression impairs cyanocobalamin absorption. Screen if symptomatic (fatigue, neuropathy, macrocytosis).
  • Bone DensityPer osteoporosis guidelines
    Trigger-based    FDA class-wide warning; greatest risk with long-term high-dose use. Ensure adequate calcium and vitamin D.
  • Chromogranin AStop PPI ≥14 days before testing
    Trigger-based    PPIs elevate CgA levels, causing false-positive results for neuroendocrine tumors.
  • Renal FunctionIf new symptoms on long-term use
    Trigger-based    Acute interstitial nephritis is a rare PPI class effect; evaluate creatinine if new renal symptoms.
CI

Contraindications & Cautions

Absolute Contraindications

  • Hypersensitivity to substituted benzimidazoles or any excipient: Includes esomeprazole, omeprazole, lansoprazole, pantoprazole, rabeprazole, and dexlansoprazole. Reactions include anaphylaxis, angioedema, bronchospasm, acute interstitial nephritis, and urticaria.
  • Rilpivirine-containing products: Elevated gastric pH drastically reduces rilpivirine absorption, risking HIV treatment failure and resistance.

Relative Contraindications (Specialist Input Recommended)

  • Concurrent clopidogrel: FDA PI states to avoid concomitant use. If acid suppression essential, consider pantoprazole or H2RA.
  • Severe hepatic impairment (Child-Pugh C): Exposure substantially increased; max 20 mg QD for most indications; 20 mg BID starting dose for ZE syndrome.

Use with Caution

  • Long-term use without clear indication: Reassess regularly. Risk of C. difficile, hypomagnesemia, B12 deficiency, fractures, fundic gland polyps, and severe cutaneous reactions.
  • Patients at osteoporosis risk: Use lowest effective dose; ensure calcium/vitamin D supplementation.
  • Suspected gastric malignancy: Symptomatic improvement does not exclude malignancy; complete endoscopic evaluation before long-term therapy.
FDA Class-Wide Regulatory Warning PPI-Associated Fracture Risk and Severe Cutaneous Adverse Reactions

The FDA issued class-wide warnings for PPIs regarding (1) possible increased risk of hip, wrist, and spine fractures with long-term, high-dose use (2010/2011) and (2) severe cutaneous adverse reactions including SJS, TEN, DRESS, and AGEP (2017 update for esomeprazole). Discontinue esomeprazole immediately at the first signs or symptoms of severe skin reactions. Use the lowest dose and shortest duration appropriate to the clinical condition.

Pt

Patient Counselling

Purpose of Therapy

Esomeprazole reduces stomach acid to help heal ulcers, relieve heartburn, protect the esophagus from acid damage, and prevent stomach ulcers caused by anti-inflammatory medications. It works best when taken consistently before meals.

How to Take

Take esomeprazole at least one hour before a meal, preferably in the morning. Swallow the capsule whole with water. If you cannot swallow the capsule, open it and sprinkle the granules on a tablespoon of applesauce, then swallow immediately without chewing. For the oral suspension, mix the packet contents with water as directed and drink within 30 minutes.

Duration of Use
Tell patientEsomeprazole is generally prescribed for 4–8 weeks. Do not continue indefinitely without medical supervision. Over-the-counter use should not exceed 14 days without consulting a healthcare provider.
Call prescriberIf symptoms persist after completing the course, or if symptoms return after stopping.
Alarm Symptoms
Tell patientHeartburn can sometimes mask serious conditions. Watch for warning signs.
Call prescriberImmediately if you experience difficulty swallowing, vomiting blood, black or bloody stools, unexplained weight loss, or chest pain.
Diarrhea
Tell patientThis medication may increase the risk of a bowel infection called C. difficile.
Call prescriberIf you develop persistent watery diarrhea, stomach pain, or fever.
Skin Reactions
Tell patientRarely, esomeprazole can cause serious skin reactions. Report any new rash or skin changes immediately.
Call prescriberImmediately if you develop a rash with blistering, peeling skin, mouth sores, or feeling unwell with a fever.
Drug Interactions
Tell patientEsomeprazole can interact with blood thinners (especially clopidogrel), seizure medications, HIV drugs, and antifungals. Always tell your healthcare providers about all medications you take.
Call prescriberBefore starting any new medication, especially if you also take a blood thinner.
Ref

Sources

Regulatory (PI / SmPC)
  1. NEXIUM (esomeprazole magnesium) delayed-release capsules / for delayed-release oral suspension. Full Prescribing Information. AstraZeneca. Revised 2023. FDA Label (2023)Primary reference for all oral dosing, indications, adverse reactions, drug interactions, and pharmacokinetic data.
  2. NEXIUM (esomeprazole magnesium). DailyMed. Updated December 2025. DailyMedMost current version of the branded label with updated dosing table and safety information.
Key Clinical Trials
  1. Richter JE, Kahrilas PJ, Johanson J, et al. Efficacy and safety of esomeprazole compared with omeprazole in GERD patients with erosive esophagitis: a randomized controlled trial. Am J Gastroenterol. 2001;96(3):656-665. doi:10.1111/j.1572-0241.2001.03600.xHead-to-head trial establishing esomeprazole 40 mg superiority over omeprazole 20 mg for erosive esophagitis healing.
  2. Kahrilas PJ, Falk GW, Johnson DA, et al. Esomeprazole improves healing and symptom resolution as compared with omeprazole in reflux oesophagitis patients. Aliment Pharmacol Ther. 2000;14(10):1249-1258. doi:10.1046/j.1365-2036.2000.00844.xEarly comparative trial showing improved healing rates with esomeprazole vs omeprazole in severe EE.
  3. Goldstein JL, Johanson JF, Suchower LJ, et al. Healing of gastric ulcers with esomeprazole versus ranitidine in patients who continued to receive NSAID therapy. Am J Gastroenterol. 2005;100(12):2650-2657. doi:10.1111/j.1572-0241.2005.00328.xKey trial supporting the NSAID-associated gastric ulcer prevention indication.
  4. Scheiman JM, Yeomans ND, Talley NJ, et al. Prevention of ulcers by esomeprazole in at-risk patients using non-selective NSAIDs and COX-2 inhibitors. Am J Gastroenterol. 2006;101(4):701-710. doi:10.1111/j.1572-0241.2006.00499.xEstablished esomeprazole 20 and 40 mg for NSAID gastroprotection in at-risk populations.
Guidelines
  1. Katz PO, Dunbar KB, Schnoll-Sussman FH, et al. ACG Clinical Guideline for the Diagnosis and Management of Gastroesophageal Reflux Disease. Am J Gastroenterol. 2022;117(1):27-56. doi:10.14309/ajg.0000000000001538Current ACG GERD guideline with PPI dosing, step-down, and long-term management recommendations.
  2. Chey WD, Leontiadis GI, Howden CW, et al. ACG Clinical Guideline: Treatment of Helicobacter pylori Infection. Am J Gastroenterol. 2017;112(2):212-239. doi:10.1038/ajg.2016.563ACG guideline recommending PPI-based triple or quadruple therapy for H. pylori eradication.
  3. Farrell B, Pottie K, Thompson W, et al. Deprescribing proton pump inhibitors. Can Fam Physician. 2017;63(5):354-364. PMID:28500192Evidence-based deprescribing guideline for PPI reduction or cessation in patients without high-risk indications.
Mechanistic / Basic Science
  1. Sachs G, Shin JM, Howden CW. Review article: the clinical pharmacology of proton pump inhibitors. Aliment Pharmacol Ther. 2006;23(Suppl 2):2-8. doi:10.1111/j.1365-2036.2006.02943.xAuthoritative review of irreversible H+/K+-ATPase inhibition and the pharmacologic basis for PPI efficacy.
Pharmacokinetics / Special Populations
  1. Dean L, Kane M. Omeprazole Therapy and CYP2C19 Genotype. In: Pratt VM, et al., editors. Medical Genetics Summaries. Bethesda (MD): NCBI; 2021. NBK100895CPIC/DPWG pharmacogenomic review covering CYP2C19 allele-specific effects on both omeprazole and esomeprazole.
  2. FDA Drug Safety Communication: Possible increased risk of fractures of the hip, wrist, and spine with the use of proton pump inhibitors. FDA. Revised March 2011. FDA.govFDA class-wide safety communication on PPI-associated fracture risk.
  3. FDA Drug Safety Communication: Low magnesium levels can be associated with long-term use of proton pump inhibitor drugs. FDA. Revised March 2011. FDA.govFDA safety communication on PPI-associated hypomagnesemia.