Metoclopramide: Comprehensive Drug Monograph

Pharmacokinetic Profile

Half-Life

5–6 h (normal renal function)

Bioavailability

80% ± 15.5% (oral)

Protein Binding

~30%

Volume of Distribution

~3.5 L/kg

Metabolism

Hepatic (CYP2D6, N-4 sulphate conjugation)

Clinical Information

Drug Class

D2 Antagonist / Prokinetic / Antiemetic

Available Doses

5 mg, 10 mg tablets; ODT; 5 mg/5 mL soln; 5 mg/mL injection

Route

PO, IV, IM, intranasal (Gimoti)

Renal Adjustment

Required (CrCl ≤60 mL/min)

Hepatic Adjustment

Required (Child-Pugh B or C)

Pregnancy

No evidence of harm in large cohort studies; may affect fetus late in pregnancy

Lactation

Excreted in breast milk; use with caution

Black Box Warning

Yes — tardive dyskinesia

Max Duration

12 weeks (all indications)

Generic Available

Yes

Indications

Indication	Approved Population	Therapy Type	Status
Symptomatic gastroesophageal reflux (documented, unresponsive to conventional therapy)	Adults	Treatment (4–12 weeks)	FDA Approved
Acute and recurrent diabetic gastroparesis	Adults	Symptomatic relief (2–8 weeks)	FDA Approved

Metoclopramide is one of the few FDA-approved drugs for diabetic gastroparesis and is listed on the WHO Model List of Essential Medicines. It functions as both a prokinetic agent (accelerating gastric emptying) and an antiemetic (via central dopamine D2 receptor blockade in the chemoreceptor trigger zone). The drug is not recommended for pediatric use due to the increased risk of extrapyramidal symptoms and methemoglobinemia in neonates. Treatment should not exceed 12 weeks due to the risk of potentially irreversible tardive dyskinesia.

Off-Label Uses

Prevention of chemotherapy-induced nausea and vomiting (CINV) — Evidence quality: Moderate. Used at higher doses (1–2 mg/kg IV) before 5-HT3 antagonists became available; now largely replaced by ondansetron and NK1 antagonists but still used in some protocols.

Prevention of postoperative nausea and vomiting (PONV) — Evidence quality: High. 10–20 mg IV/IM near end of surgery; established efficacy but EPS risk limits use as first-line agent.

Migraine-associated nausea and vomiting — Evidence quality: Moderate. 10 mg IV in ED settings; improves gastric absorption of co-administered oral analgesics.

Nausea and vomiting of pregnancy — Evidence quality: Moderate. Used as second-line agent; large cohort studies show no evidence of teratogenicity.

Small bowel intubation facilitation — Evidence quality: Moderate. 10 mg IV to accelerate passage of nasogastric/intestinal tubes through the pylorus.

Radiologic GI procedures — Evidence quality: Moderate. Accelerates barium transit; prevents vomiting after oral barium ingestion.

Dose

Dosing

Adult Dosing by Clinical Scenario

Clinical Scenario	Starting Dose	Maintenance Dose	Maximum Dose	Notes
GERD — continuous therapy	10–15 mg PO QID	10–15 mg QID for 4–12 weeks	60 mg/day	30 min before each meal and at bedtime Duration determined by endoscopic response; do not exceed 12 weeks
GERD — intermittent (situational) therapy	Up to 20 mg PO × 1	Single dose before provoking situation	20 mg per dose	Use when symptoms occur only at specific times Consider dosage reductions in special populations
Diabetic gastroparesis — acute/recurrent	10 mg PO QID	10 mg QID for 2–8 weeks	40 mg/day	30 min before each meal and at bedtime If unable to take oral, use IV/IM for up to 10 days then switch to PO
PONV prophylaxis (off-label)	10–20 mg IV/IM × 1	Single dose	20 mg	Given near end of surgery IM preferred at end of procedure
Small bowel intubation facilitation (off-label)	10 mg IV × 1	Single dose	10 mg	Given over 1–2 minutes

Special Population Dosing Adjustments

Population	GERD Dose	Gastroparesis Dose	Maximum Dose	Notes
Elderly (≥65 years)	5 mg QID (start)	5 mg QID (start)	Titrate to adult dose if tolerated	Increased sensitivity to TD and parkinsonian effects Elderly women at highest TD risk
Moderate–severe hepatic impairment (Child-Pugh B/C)	5 mg QID or 10 mg TID	5 mg QID	30 mg/day (GERD); 20 mg/day (gastroparesis)	Reduced clearance
Renal impairment (CrCl ≤60 mL/min)	5 mg QID or 10 mg BID	5 mg BID	20 mg/day (GERD); 10 mg/day (gastroparesis)	Clearance reduced ~50%; t½ prolonged
ESRD (HD or CAPD)	5 mg QID or 10 mg BID	5 mg BID	20 mg/day (GERD); 10 mg/day (gastroparesis)	Dialysis removes relatively little drug
CYP2D6 poor metabolizers	5 mg QID or 10 mg BID	5 mg BID	20 mg/day (GERD); 10 mg/day (gastroparesis)	Same reductions as renal impairment
Concomitant strong CYP2D6 inhibitors	5 mg QID or 10 mg BID	5 mg BID	20 mg/day (GERD); 10 mg/day (gastroparesis)	Inhibitors: quinidine, bupropion, fluoxetine, paroxetine
Pediatric	Not recommended			Increased EPS risk; methemoglobinemia in neonates Not FDA-approved for pediatric use

Clinical Pearl: The 12-Week Rule

Treatment with metoclopramide should not exceed 12 weeks for any indication. The risk of tardive dyskinesia increases with both duration and cumulative dose. For GERD, duration is determined by endoscopic response (4–12 weeks). For diabetic gastroparesis, 2–8 weeks is typical. If symptoms recur after stopping, carefully weigh the benefit of re-treatment against TD risk. Patients with diabetes are at increased risk for TD.

Pharmacology

Mechanism of Action

Metoclopramide exerts its clinical effects through multiple receptor interactions. As a dopamine D2 receptor antagonist, it blocks dopaminergic signaling in the chemoreceptor trigger zone of the area postrema, producing its central antiemetic effect. Peripherally, D2 receptor antagonism in the gastrointestinal tract, combined with 5-HT4 receptor agonism and sensitization of muscarinic receptors on smooth muscle, underlies its prokinetic action. Metoclopramide increases the tone and amplitude of gastric antral contractions, relaxes the pyloric sphincter and duodenal bulb, and accelerates peristalsis through the duodenum and jejunum. It also raises resting lower esophageal sphincter pressure in a dose-dependent fashion (effects observed from 5 mg, lasting up to 2–3 hours at 20 mg). At higher doses, 5-HT3 receptor antagonism may contribute additional antiemetic activity. The prokinetic effect does not depend on intact vagal innervation but can be abolished by anticholinergic drugs. Metoclopramide has little effect on colonic or gallbladder motility and does not stimulate gastric, biliary, or pancreatic secretions.

ADME Profile

Parameter	Value	Clinical Implication
Absorption	Rapidly and well absorbed; Tmax 1–2 h; oral bioavailability 80% ± 15.5% (variable first-pass, range 32–100%)	Administer 30 min before meals to coincide with peak prokinetic activity at mealtime
Distribution	Vd ~3.5 L/kg; protein binding ~30%; lipid-soluble; crosses blood–brain barrier	High Vd indicates extensive tissue distribution; CNS penetration underlies both antiemetic efficacy and neuropsychiatric side effects
Metabolism	Hepatic via CYP2D6 and N-4 sulphate conjugation; minimal hepatic metabolism in injection PI described as “simple conjugation”	CYP2D6 poor metabolizers and patients on strong CYP2D6 inhibitors require dose reduction; safe in advanced liver disease if renal function is normal
Elimination	~85% excreted in urine within 72 h (half as free or conjugated drug); t½ 5–6 h (normal renal function); clearance reduced ~50% in renal impairment	Dose reduction required when CrCl ≤60 mL/min; dialysis removes relatively little drug

Side Effects

Metoclopramide has a significant adverse effect profile dominated by CNS and extrapyramidal reactions. The incidence of adverse reactions correlates with dose and duration of therapy.

≥10%Very Common

Adverse Effect	Incidence	Clinical Note
Restlessness (akathisia)	~10%	Motor restlessness with anxiety, agitation, jitteriness, inability to sit still, pacing, and foot tapping; may resolve with dose reduction
Drowsiness	~10%	May impair ability to drive or operate machinery; additive with CNS depressants
Fatigue / lassitude	~10%	CNS depressant effect; may manifest as over-sedation in elderly

1–10%Common

Adverse Effect	Incidence	Clinical Note
Insomnia	<10%	Less frequent than drowsiness; CNS stimulatory effect in some patients
Headache	<10%	May also occur as withdrawal symptom
Dizziness	<10%	Also reported during withdrawal
Diarrhea	<10%	Related to prokinetic effect on intestinal transit

SeriousSerious (Regardless of Frequency)

Adverse Effect	Estimated Frequency	Typical Onset	Required Action
Tardive dyskinesia (TD)	Risk increases with duration & dose; higher in elderly women & diabetics	Months of treatment; can occur earlier	Immediately discontinue; no known effective treatment; may be irreversible; do not restart
Acute dystonic reactions (torticollis, oculogyric crisis, trismus)	More common at 30–40 mg/day and in adults <30 years	First 24–48 hours	Diphenhydramine 25–50 mg IV/IM or benztropine 1–2 mg IV/IM; discontinue metoclopramide
Drug-induced parkinsonism	Dose-dependent	Commonly within first 6 months; can occur later	Discontinue; symptoms generally subside within 2–3 months; do not add antiparkinsonian agents before stopping metoclopramide
Neuroleptic malignant syndrome (NMS)	Rare	Any time; especially with concomitant antipsychotics or overdose	Discontinue immediately; intensive supportive care; dantrolene or bromocriptine may be considered
Depression with suicidal ideation/suicide	Uncommon	Any time during treatment	Avoid in patients with history of depression; discontinue if depressive symptoms emerge
Hyperprolactinemia (galactorrhea, amenorrhea, gynecomastia, impotence)	Uncommon	Weeks to months	Discontinue if clinically significant; check prolactin level
Hypertensive crisis (pheochromocytoma)	Very rare (contraindicated in pheochromocytoma)	Minutes after administration	Treat hypertensive emergency; screen for pheochromocytoma; metoclopramide is contraindicated
Methemoglobinemia (neonates)	Rare; overdose in neonates	Hours after overdose	Methylene blue; neonates have reduced NADH-cytochrome b5 reductase

DiscontinuationDiscontinuation Rates

Neurologic Adverse Effects

Key driver

TD, EPS, and parkinsonian symptoms are the primary reasons for treatment discontinuation. TD may be irreversible even after stopping. Akathisia and drowsiness also limit tolerability.

Withdrawal Symptoms

Reported

Dizziness, nervousness, and headaches have been reported in a small number of patients after stopping metoclopramide. Nervous system effects may also emerge after discontinuation.

Critical: Recognizing Tardive Dyskinesia

TD presents as involuntary, repetitive, purposeless movements most commonly involving the face and tongue (lip smacking, puckering, chewing, tongue protrusion, grimacing) but can also affect the trunk and extremities. Movements may be choreoathetotic. Metoclopramide itself can mask TD by suppressing the movements, only for them to become apparent upon dose reduction or discontinuation. There is no known effective treatment for established TD. The prescriber must actively screen for early signs at each visit and immediately discontinue metoclopramide at the first sign of involuntary movements.

Int

Drug Interactions

Metoclopramide’s interactions are primarily pharmacodynamic (additive CNS and extrapyramidal effects) and pharmacokinetic (CYP2D6 substrate, altered GI absorption of co-administered drugs due to prokinetic effect).

MajorAntipsychotics (typical and atypical)

MechanismAdditive dopamine D2 receptor blockade

EffectIncreased risk of TD, EPS, and NMS

ManagementAvoid concomitant use

FDA PI

MajorMAO inhibitors

MechanismMetoclopramide releases catecholamines; MAOIs prevent catecholamine degradation

EffectRisk of hypertensive crisis

ManagementAvoid concomitant use

FDA PI

MajorCNS depressants (opioids, benzodiazepines, alcohol)

MechanismAdditive CNS depression

EffectExcessive sedation, drowsiness, impaired psychomotor function

ManagementAvoid concomitant use; monitor for adverse reactions if unavoidable

FDA PI

ModerateStrong CYP2D6 inhibitors (quinidine, fluoxetine, paroxetine, bupropion)

MechanismInhibition of CYP2D6-mediated metoclopramide metabolism

EffectIncreased metoclopramide exposure; increased risk of EPS and other adverse effects

ManagementReduce metoclopramide dose per FDA PI special population tables

FDA PI

ModerateAnticholinergic drugs

MechanismAnticholinergics oppose metoclopramide’s prokinetic muscarinic sensitization

EffectReduced prokinetic efficacy of metoclopramide

ManagementAvoid combining if prokinetic effect is the therapeutic goal

FDA PI

ModerateInsulin and oral hypoglycemics

MechanismAccelerated gastric emptying changes the timing of food delivery to the intestine

EffectAltered glucose absorption kinetics; potential hypoglycemia if insulin acts before food is absorbed

ManagementAdjust insulin timing or dosage; increased blood glucose monitoring when starting or stopping metoclopramide

FDA PI

MinorDrugs absorbed in the stomach vs. small intestine

MechanismAccelerated gastric emptying decreases absorption of drugs requiring prolonged gastric contact and increases absorption of drugs absorbed in the small intestine

EffectMay reduce digoxin absorption; may increase cyclosporine absorption

ManagementMonitor drug levels for narrow-therapeutic-index medications

FDA PI

Mon

Monitoring

Tardive Dyskinesia ScreeningEvery visit; at minimum monthly
RoutineActively assess for involuntary movements of face, tongue, trunk, and extremities at every encounter. Use a standardized tool (AIMS) if available. Discontinue immediately at first sign of TD. Risk increases with duration >12 weeks, higher cumulative dose, elderly age, female sex, and diabetes.
Extrapyramidal SymptomsFirst 48 hours; then ongoing
RoutineAcute dystonia typically occurs within 24–48 hours of starting therapy; parkinsonian symptoms may develop within the first 6 months. Akathisia can occur at any time. Treat acute dystonia with diphenhydramine or benztropine. Discontinue metoclopramide for any EPS.
Mental Status / MoodEach visit
RoutineScreen for depression, suicidal ideation, confusion, and cognitive changes. Avoid use in patients with prior history of depression. Sedation may manifest as confusion and over-sedation in the elderly.
Renal FunctionBaseline; periodically
RoutineClearance reduced ~50% in renal impairment. Reassess creatinine clearance if renal function changes; adjust dose accordingly. Drug substantially excreted by the kidney.
Blood GlucoseOngoing in diabetic patients
Trigger-basedMetoclopramide accelerates gastric emptying, altering the timing of food delivery to the intestine. Insulin dosing or timing may need adjustment to prevent hypoglycemia in diabetic patients using metoclopramide for gastroparesis.
Treatment DurationAt each prescribing encounter
RoutineDo not exceed 12 weeks total. Periodically reassess the need for continued treatment. Document the clinical rationale and patient informed consent regarding TD risk at each renewal.

Contraindications & Cautions

Absolute Contraindications

History of tardive dyskinesia or dystonic reaction to metoclopramide
GI conditions where stimulation of motility is dangerous — hemorrhage, mechanical obstruction, or perforation
Pheochromocytoma or catecholamine-releasing paragangliomas — risk of hypertensive crisis from catecholamine release
Epilepsy — may increase frequency and severity of seizures
Hypersensitivity to metoclopramide — laryngeal/glossal angioedema and bronchospasm reported

Relative Contraindications (Specialist Input Recommended)

Parkinson’s disease — dopamine D2 antagonism may worsen parkinsonian symptoms; avoid use
History of depression — depression with suicidal ideation reported; avoid use if possible

Use with Caution

Elderly patients (especially women) — highest risk group for TD; start at 5 mg QID
Diabetes mellitus — increased TD risk; insulin dosing adjustments may be needed due to altered gastric emptying
Renal impairment (CrCl ≤60 mL/min) — dose reduction required; risk of toxicity from drug accumulation
Congestive heart failure or cirrhosis — transient aldosterone increase may cause fluid retention and volume overload
Hypertension — metoclopramide can release catecholamines; avoid with MAO inhibitors
NADH-cytochrome b5 reductase deficiency — increased risk of methemoglobinemia
CYP2D6 poor metabolizers — dose reduction required (same as renal impairment dosing)

FDA Boxed Warning Tardive Dyskinesia

Metoclopramide can cause tardive dyskinesia (TD), a serious movement disorder that is often irreversible. There is no known treatment for TD. The risk of developing TD increases with duration of treatment and total cumulative dosage. Discontinue metoclopramide in patients who develop signs or symptoms of TD. In some patients, symptoms may lessen or resolve after metoclopramide is stopped. Avoid treatment with metoclopramide for longer than 12 weeks because of the increased risk of developing TD with longer-term use.

Patient Counselling

Purpose of Therapy

Metoclopramide helps your stomach empty food more quickly and reduces nausea and vomiting. It is prescribed for a limited period — usually no longer than 12 weeks — because of the risk of a serious, potentially permanent side effect affecting involuntary movements.

How to Take

Take metoclopramide 30 minutes before each meal and at bedtime. If using the orally disintegrating tablet (ODT), place it on your tongue and let it dissolve, then swallow. Do not take this medication for longer than your doctor has prescribed.

Tardive Dyskinesia (Critical Warning)

Tell patientThis medication can rarely cause involuntary movements of the face, tongue, or body that may become permanent, even after stopping the drug. The risk increases the longer you take it and at higher doses. Do not take metoclopramide for longer than prescribed.

Call prescriberImmediately if you notice any uncontrollable movements of your face, tongue, lips (such as lip smacking, puckering, chewing motions, tongue protrusion), or any other unusual involuntary movements.

Drowsiness and Impaired Alertness

Tell patientMetoclopramide can cause drowsiness and fatigue, especially when combined with alcohol, sedatives, or pain medications. Avoid driving or operating heavy machinery until you know how this medication affects you.

Call prescriberIf drowsiness is severe, does not improve, or if you experience confusion.

Restlessness and Muscle Stiffness

Tell patientYou may experience a feeling of inner restlessness, an inability to sit still, or muscle stiffness. These side effects are more common in younger adults and at higher doses.

Call prescriberIf you develop muscle spasms (especially of the neck, face, or tongue), difficulty speaking or swallowing, or a feeling that your eyes are pulling upward. These symptoms need prompt treatment.

Mood Changes

Tell patientSome patients experience low mood or depression while taking metoclopramide. If you have a history of depression, discuss this with your doctor before starting.

Call prescriberIf you feel unusually sad, hopeless, lose interest in daily activities, or have any thoughts of harming yourself.

Diabetes Management

Tell patientIf you have diabetes, metoclopramide changes how quickly your stomach empties food. This may affect your blood sugar levels. Monitor your blood glucose more closely, especially after starting or stopping this medication.

Call prescriberIf you experience frequent low blood sugar episodes (shakiness, sweating, confusion) or if your blood sugar is consistently higher or lower than usual.

Ref

Sources

Regulatory (PI / SmPC)

Reglan (metoclopramide) Tablets — FDA-Approved Prescribing Information, revised August 2017. ANI Pharmaceuticals. FDA Label (Tablets)Current FDA-approved label for Reglan tablets; source for indications, boxed warning, dosing tables for GERD and gastroparesis including special population adjustments, and adverse reactions.
Reglan Injection (metoclopramide injection, USP) — FDA-Approved Prescribing Information, revised 2010. Baxter/ESI Lederle. FDA Label (Injection)FDA-approved label for metoclopramide injection; includes IV/IM dosing for PONV, small bowel intubation, and pharmacokinetic data (Vd 3.5 L/kg, protein binding ~30%, t½ 5–6 h).
FDA Drug Safety Communication: FDA Requires Boxed Warning and Risk Mitigation Strategy for Metoclopramide-Containing Drugs, 2009. FDA Safety PageFDA communication mandating boxed warning for tardive dyskinesia risk and treatment duration limitation of 12 weeks.

Key Clinical Trials

Parkman HP, Hasler WL, Fisher RS, et al. American Gastroenterological Association technical review on the diagnosis and treatment of gastroparesis. Gastroenterology. 2004;127(5):1592–1622. PubMed: 15521026AGA comprehensive technical review positioning metoclopramide as a first-line prokinetic for gastroparesis with discussion of efficacy evidence and TD risk.
Rao AS, Camilleri M. Review article: metoclopramide and tardive dyskinesia. Aliment Pharmacol Ther. 2010;31(1):11–19. PubMed: 19886950Key review quantifying the risk of tardive dyskinesia with metoclopramide and identifying risk factors including age, sex, diabetes, and treatment duration.
Matok I, Gorodischer R, Koren G, et al. The safety of metoclopramide use in the first trimester of pregnancy. N Engl J Med. 2009;360(24):2528–2535. PubMed: 19516033Large Israeli cohort study (over 81,000 deliveries) finding no increased risk of congenital malformations, low birth weight, preterm delivery, or perinatal mortality with first-trimester metoclopramide exposure.

Guidelines

Camilleri M, Parkman HP, Shafi MA, et al. Clinical Guideline: Management of Gastroparesis. Am J Gastroenterol. 2013;108(1):18–37. PubMed: 23147521ACG clinical guideline recommending metoclopramide as first-line pharmacotherapy for gastroparesis with strong emphasis on limiting treatment duration.
Gan TJ, Belani KG, Bergese S, et al. Fourth Consensus Guidelines for the Management of Postoperative Nausea and Vomiting. Anesth Analg. 2020;131(2):411–448. PubMed: 32467512Consensus PONV guideline including metoclopramide 25–50 mg as a perioperative antiemetic option with discussion of EPS risk.

Mechanistic / Basic Science

Sanger GJ, Andrews PLR. A History of Drug Discovery for Treatment of Nausea and Vomiting and the Implications for Future Research. Front Pharmacol. 2018;9:913. PubMed: 30233361Historical review of antiemetic pharmacology covering metoclopramide’s role as a D2 antagonist, 5-HT3 antagonist, and 5-HT4 agonist in the context of evolving antiemetic therapy.
Lee A, Kuo B. Metoclopramide in the treatment of diabetic gastroparesis. Expert Rev Endocrinol Metab. 2010;5(5):653–662. PubMed: 21278804Expert review of metoclopramide’s prokinetic mechanism, clinical efficacy in diabetic gastroparesis, and comparison with alternative prokinetics.

Pharmacokinetics / Special Populations

Bateman DN. Clinical pharmacokinetics of metoclopramide. Clin Pharmacokinet. 1983;8(6):523–529. PubMed: 6360466Foundational PK review: oral bioavailability 32–100% (variable first-pass), clearance reduced ~50% in renal failure, N-4 sulphate conjugation as major metabolic pathway.
McGovern EM, Grevel J, Bryson SM. Pharmacokinetics of high-dose metoclopramide in cancer patients. Clin Pharmacokinet. 1986;11(6):415–424. PubMed: 3542335PK study of high-dose metoclopramide in oncology patients demonstrating linear kinetics at antiemetic doses and establishing accumulation patterns.
Ge S, Mendley SR, Gerhart JG, et al. Population Pharmacokinetics of Metoclopramide in Infants, Children, and Adolescents. Clin Transl Sci. 2020;13(6):1189–1198. PubMed: 32324313Population PK study in pediatric patients demonstrating age-dependent clearance and supporting the caution against pediatric use due to variable drug exposure.