Geodon
Ziprasidone
Generic Name
Ziprasidone
Mechanism
- Ziprasidone is a second‑generation antipsychotic.
- Binding profile:
- *High affinity* for dopamine D₂ and serotonin 5‑HT₂A receptors → reduces psychotic symptoms.
- *Partial agonist* at 5‑HT₁A receptors → contributes to anxiolytic and antidepressant effects.
- *Low affinity* for histamine H₁, muscarinic M₁/M₃, and adrenergic α₁ receptors → minimal sedation and anticholinergic burden.
- Neurochemical impact: D₂ blockade in the mesolimbic pathway dampens positive symptoms; 5‑HT₂A blockade modulates negative and cognitive symptoms.
- Cardiac effect: Inhibits HERG potassium channels → can prolong QTc interval.
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Pharmacokinetics
- Absorption: Bioavailability ~9 % (oral); significantly reduced by food (fatty meals).
- Distribution: Highly protein‑bound (~95 %); crosses the blood‑brain barrier.
- Metabolism: Predominantly hepatic via CYP3A4; minor CYP2D6 contribution.
- Elimination: Renal excretion of unchanged drug & metabolites; half‑life ~7–12 h (oral).
- Drug interactions:
- Strong CYP3A4 inhibitors ↑ plasma levels (e.g., ketoconazole) → ↑ QTc risk.
- CYP3A4 inducers ↓ exposure (e.g., rifampin, carbamazepine).
- Concomitant drugs capable of prolonging QTc (e.g., amiodarone) should be avoided or monitored.
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Indications
- Schizophrenia (acute and maintenance).
- Bipolar Disorder (acute mania).
- Adjunctive therapy in treatment‑resistant schizophrenia (per FDA guidance).
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Contraindications
- Contraindicated in patients with:
- Known hypersensitivity to ziprasidone.
- Baseline QTc > 460 ms (men) / > 470 ms (women).
- Severe hepatic impairment.
- Warnings:
- QTc prolongation & torsades de pointes, especially with electrolyte disturbances, bradycardia, or concomitant QT‑prolonging drugs.
- Falls/orthostatic hypotension in elderly.
- Weight‑neutral: still monitor metabolic parameters.
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Dosing
| Condition | Initial Dose | Titration | Maintenance | Notes |
| Schizophrenia | 20 mg PO BID (fasting) | +20 mg/day increments up to 80 mg BID | 50–80 mg BID (total 100–160 mg/day) | Avoid food within 1 h prior to ingestion. |
| Bipolar Mania | 20 mg PO BID | +20 mg/day up to 80 mg BID | 60–80 mg BID | Rapid titration may precipitate mania; monitor mood. |
• Intravenous: 2 mg/kg over 5 min, then 1 mg/kg/12 h. Not first‑line for chronic use.
• Swallowing difficulties: Chewable tablets or oral solution; avoid crushing.
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Adverse Effects
Common (≥10 %)
• Akathisia, dystonia (rare).
• Extrapyramidal symptoms (≤5 %).
• Metabolic: weight gain, dyslipidemia (low‑)
• Dry mouth, constipation, constipation → monitor GI motility.
Serious (≤1 %)
• QTc prolongation → torsades de pointes.
• Neuroleptic malignant syndrome (rare).
• Severe agitation, lability.
• Hepatic dysfunction → AST/ALT rise.
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Monitoring
| Parameter | Frequency | Target |
| QTc | Baseline → 1 wk → 4 wk → every 3 mo (if stable) | < 460 ms (M)/470 ms (F); < 500 ms acceptable with close surveillance |
| Lipid profile, fasting glucose | Baseline → every 3 mo | < 200 mg/dL |
| Weight & BMI | Baseline → every 3 mo | maintain < 30 kg/m² |
| LFTs | Baseline → every 3 mo | < two‑fold ULN |
| ECG (if QTc ≥ 460 ms) | Repeat 1 wk | Evaluate need to discontinue or adjust |
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Clinical Pearls
- Take with an empty stomach – a fatty meal can cut bioavailability by >50 %. Consider administering in the morning uncoupled from meals.
- Avoid nocturnal dosing – peak dose at night → increased risk of nocturnal QTc prolongation.
- Monitor electrolytes – K⁺ < 3.5 mEq/L, Mg²⁺ < 1.5 mEq/L augment torsades risk.
- Switching from other antipsychotics: hold previous D₂ blocker for 4–5 half‑lives to prevent neuroleptic syndrome.
- High‑yield ECOG: Ziprasidone is unique among atypicals for its minimal metabolic effects yet significant QTc liability – a classic “protect ketosis, risk arrhythmia” scenario.
- Pediatric use: FDA approved for ≤ 18 y with schizophrenia; dose starts 5 mg PO BID and titrates to ≤ 30 mg BID.
- Pregnancy: Category C – weigh psychiatric stability against fetal QTc prolongation risk; counsel patient.
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