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  • Educational Only: Not for clinical decision-making.
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Bedside Snapshot
  • Core ED/IM dose: 10–20 mg IM single dose; may repeat 10 mg q2h or 20 mg q4h; maximum 40 mg/day (IM use typically ≤3 days).
  • Onset / peak: IM onset ~15–30 min; peak ~45–60 min; clinically useful effect often 2–4 hours.
  • Key danger: Dose- and concentration-dependent QTc prolongation → torsades risk; avoid in patients with baseline long QT or strong QT-prolonging polypharmacy.
  • Special: IM only for parenteral use — do NOT give IV. When converting to oral, give with a ≥500 kcal meal to ensure adequate absorption.
Brand & Generic Names
  • Generic: Ziprasidone
  • Brand: Geodon (U.S.); Zeldox (selected regions)
Medication Class

Second‑generation (atypical) antipsychotic — dopamine D2 and serotonin 5‑HT2A receptor antagonist with additional serotonin/norepinephrine reuptake inhibition; sedative/α1 effects contribute to calming but increase orthostatic hypotension risk.

Pharmacology

Mechanism of Action:

  • D2 receptor antagonism → reduces positive psychotic symptoms and agitation.
  • 5‑HT2A antagonism → relative EPS sparing and contribution to antipsychotic effects.
  • 5‑HT1A partial agonism and activity at other serotonin receptors → anxiolytic/antimanic effects.
  • Moderate SERT/NET inhibition → minor antidepressant/anxiolytic contribution for maintenance therapy.
  • H1 and α1 antagonism → sedation and orthostatic hypotension (relevant for ED/IM use).
  • Blocks cardiac IKr (hERG) channels → QTc prolongation risk (dose/concentration dependent).

Pharmacokinetics:

  • IM absorption: near-complete bioavailability; onset ~15–30 min; Tmax ~45–60 min; clinical effect often 2–4 hours.
  • Oral: ~60% bioavailability when taken with a ≥500 kcal meal; markedly reduced without food (important for transitions to PO).
  • Distribution: large Vd, high protein binding (~99%); not dialyzable in a clinically meaningful way.
  • Metabolism: aldehyde oxidase primary, CYP3A4 secondary.
  • Elimination: metabolites in feces and urine; oral half‑life ~7–10 hours (IM effective duration shorter for single doses).
Indications
  • Acute severe agitation due to psychosis or schizophrenia — rapid IM control when oral route not feasible.
  • ED/psych emergency/settings where antipsychotic sedation is preferred to benzodiazepine stacking (less respiratory depression).
  • Short-term parenteral control on inpatient/ICU when oral administration is not possible; bridge to oral therapy once stable.
  • Oral maintenance for schizophrenia or bipolar disorder (NOT ED‑first-line for long-term management without psychiatry involvement).
Dosing & Administration

Available Forms:

  • IM injection (ziprasidone mesylate) — typically reconstituted to yield 20 mg/mL (20 mg per 1 mL; 10 mg per 0.5 mL).
  • Oral capsules: 20 mg, 40 mg, 60 mg, 80 mg (used for maintenance).

Adult IM Dosing (ED/IM/Parenteral):

  • Initial: 10–20 mg IM single dose.
  • Repeat: 10 mg IM every 2 hours OR 20 mg IM every 4 hours as needed.
  • Maximum: 40 mg/day (IM); IM use studied up to 3 consecutive days only.

Adult Oral Dosing (continuation / maintenance):

  • Start 20 mg PO BID with food (≥500 kcal). Titrate to 40–80 mg PO BID as tolerated; max 160 mg/day.
Contraindications

Contraindications:

  • Known congenital long QT syndrome or baseline significant QT prolongation.
  • Recent acute myocardial infarction or uncompensated heart failure.
  • Concurrent use of contraindicated QT‑prolonging drugs per product labeling.
  • Hypersensitivity to ziprasidone or formulation components.
  • Elderly patients with dementia‑related psychosis — increased mortality (boxed warning).

Precautions (ED/IM emphasis):

  • Correct hypokalemia and hypomagnesemia before dosing when feasible; avoid use or monitor closely in polypharmacy with other QT-prolongers.
  • Monitor hemodynamics — orthostatic hypotension and syncope risk, especially in elderly or volume‑depleted patients.
  • Avoid IV administration — IM only for parenteral use.
  • Caution with concomitant CNS depressants (benzodiazepines, opioids) — additive respiratory and hemodynamic depression.
Warning: Ziprasidone has significant QTc‑prolonging potential. Obtain ECG/Evaluate QTc and correct electrolytes when feasible; avoid in patients with high baseline QT risk.
Adverse Effects

Common (short-term IM use):

  • Sedation/somnolence, dizziness, headache
  • Injection‑site pain
  • Mild orthostatic hypotension, tachycardia
  • Nausea, vomiting
  • Extrapyramidal symptoms (akathisia, mild parkinsonism, dystonia) — more likely with repeat/higher doses

Serious / ED‑relevant:

  • QT/QTc prolongation and torsades de pointes — risk increased with hypokalemia/hypomagnesemia, underlying heart disease, or QT‑prolonging polypharmacy
  • Neuroleptic malignant syndrome (NMS)
  • Tardive dyskinesia with chronic use
  • Severe cutaneous reactions (rare), agranulocytosis (rare), seizures in predisposed patients
Drug Interactions
  • QT‑prolonging agents: (e.g., amiodarone, sotalol, macrolides, fluoroquinolones) — increased torsades risk; avoid or monitor closely.
  • Strong CYP3A4 inhibitors/inducers: may alter ziprasidone exposure — review product labeling and adjust as needed for chronic therapy.
  • Concomitant CNS depressants: additive sedation and respiratory depression risk (benzodiazepines, opioids) — monitor airway and ventilation closely in ED/ICU.
Special Populations
  • Cardiac disease / electrolyte abnormalities: higher risk for torsades; avoid when possible and monitor ECG/K/Mg closely.
  • Hepatic impairment: start low and titrate carefully — hepatic dysfunction may increase free drug levels.
  • Renal impairment: no formal dose change, but monitor for amplified QT risk in uremia or electrolyte disturbance.
  • Elderly: increased risk of hypotension, falls, and cerebrovascular events — use lower doses and tighter monitoring.
Monitoring
  • ECG: baseline or early ECG in high‑risk patients and trend QTc if multiple doses are given.
  • Electrolytes: K and Mg (correct before dosing when feasible).
  • Vital signs and sedation level: monitor BP, HR, RR, SpO2 — continuous monitoring if given with other sedatives.
  • Mental status and EPS: observe for akathisia, dystonia, rigidity; treat if severe.
Clinical Pearls
IM only: Ziprasidone has NO IV formulation — do not inject intravenously.
Onset: Expect improvement in 15–30 minutes — not immediate in most cases; plan security/monitoring and reassessment windows accordingly.
QTc warning: If the patient is on other QT‑prolongers (amiodarone, sotalol, fluoroquinolones, macrolides, methadone), prioritize alternatives or rigorous cardiac monitoring.
Food effect (PO): Oral ziprasidone requires a ≥500 kcal meal for reliable absorption — plan transitions to PO with food.
References
  • 1. Bouchette, D. (2024). Ziprasidone. In StatPearls. StatPearls Publishing.
  • 2. Pfizer Inc. (2025). Geodon (ziprasidone) prescribing information.
  • 3. Citrome, L. (2009). Using oral ziprasidone effectively: the food effect and dose‑response. Journal of Clinical Psychiatry, 70(1), 58–62.
  • 4. Gandelman, K., et al. (2009). The impact of calories and fat content of meals on oral ziprasidone absorption. Journal of Clinical Psychiatry, 70(1), 58–62.
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