Quinidine Sulfate

Quinidine is a Class Ia antiarrhythmic and antimalarial agent used to treat heart rhythm disorders and Plasmodium falciparum malaria. It works by blocking sodium and potassium channels to stabilize cardiac membranes.

Dosage of Quinidine must be highly individualized based on the patient's clinical response, heart rate, and blood levels of the drug.

• For Atrial Fibrillation/Flutter (Maintenance of Sinus Rhythm): The typical adult dose of Quinidine gluconate extended-release is 324 mg to 648 mg taken every 8 to 12 hours. Healthcare providers usually start with a lower dose and titrate upward while monitoring the EKG (electrocardiogram) for changes in the QT interval.
• For Ventricular Arrhythmias: The dosage is similar to atrial rhythms, often ranging from 324 mg to 972 mg per day in divided doses.
• For Severe Malaria: This typically requires an initial 'loading dose' administered via slow intravenous infusion (e.g., 10 mg/kg over 1-2 hours) followed by a continuous maintenance infusion. This must only be performed in an intensive care or telemetry setting.

Quinidine is rarely used in pediatric populations. When required, dosing is strictly weight-based (e.g., 30 mg/kg/day in 4 to 5 divided doses for the sulfate form). However, safety and efficacy in children have not been established through large-scale clinical trials. Most pediatric use is considered off-label and must be managed by a pediatric cardiologist or infectious disease specialist.

Renal Impairment

In patients with reduced kidney function, the excretion of Quinidine and its metabolites is slowed. Healthcare providers may reduce the frequency of dosing or the total daily dose to prevent accumulation. Close monitoring of serum quinidine levels is mandatory in patients with a GFR (Glomerular Filtration Rate) below 50 mL/min.

Hepatic Impairment

Since Quinidine is primarily metabolized by the liver, patients with cirrhosis or hepatitis are at a high risk of toxicity. Dose reductions of 25% to 50% are common, and frequent liver function tests (LFTs) are required during therapy.

Elderly Patients

Older adults often have decreased volume of distribution and slower clearance. They are also more susceptible to the side effect of orthostatic hypotension (dizziness upon standing). Providers typically 'start low and go slow' with this population.

To ensure the medication works effectively and to minimize side effects, follow these guidelines:

• Consistency is Key: Take Quinidine at the same times every day to maintain a steady level in your bloodstream.
• Food vs. Empty Stomach: You may take Quinidine with food or milk if it causes stomach upset. However, you should choose one way (always with food or always without) and stick to it to keep absorption consistent.
• Swallow Whole: Do not crush, chew, or break extended-release tablets (Quinidine gluconate). Doing so can release too much medicine at once, increasing the risk of dangerous heart rhythm problems.
• Hydration: Drink plenty of fluids unless your doctor has told you to limit fluid intake due to heart failure.
• Storage: Store at room temperature (68°F to 77°F) away from moisture, light, and heat. Keep the bottle tightly closed.

If you miss a dose, take it as soon as you remember. If it is almost time for your next scheduled dose (within 4 hours), skip the missed dose and return to your regular schedule. Never double the dose to catch up, as this can lead to life-threatening cardiac toxicity.

An overdose of Quinidine is a medical emergency. Symptoms may include extreme dizziness, fainting, blurred vision, ringing in the ears (tinnitus), severe diarrhea, and a dangerously slow or irregular heartbeat. If an overdose is suspected, call 911 or your local emergency services immediately. In a hospital setting, treatment may include gastric lavage (stomach pumping), administration of sodium lactate to reverse cardiac effects, or cardiac pacing.

> Important: Follow your healthcare provider's dosing instructions exactly. Do not adjust your dose or stop taking this medication without direct medical guidance, as sudden discontinuation can cause your arrhythmia to return more severely.

Many patients taking Quinidine experience gastrointestinal issues, especially during the first few weeks of treatment. These include:

• Diarrhea: This is the most common reason for discontinuing the drug. It can be severe and may be accompanied by abdominal cramping.
• Nausea and Vomiting: Often occurring shortly after taking a dose.
• Cinchonism: A unique cluster of symptoms caused by cinchona alkaloids. Mild cinchonism includes tinnitus (ringing in the ears), slight dizziness, and blurred vision. These symptoms usually indicate that the dosage may be too high.

Quinidine is a high-alert medication that requires strict adherence to safety protocols. It has a narrow therapeutic window, meaning the difference between a dose that helps the heart and a dose that harms it is very small. Patients must be committed to regular follow-up appointments and laboratory monitoring.

WARNING: INCREASED MORTALITY. In many trials of antiarrhythmic therapy for non-life-threatening arrhythmias, these drugs (including Quinidine) have been associated with an increased risk of death compared to no treatment. Therefore, Quinidine should be reserved for patients with life-threatening ventricular arrhythmias or highly symptomatic atrial fibrillation where other treatments have failed. Your doctor will weigh this risk carefully before prescribing.

• QT Prolongation: Quinidine naturally lengthens the QT interval on an EKG. If this interval becomes too long, it can trigger a fatal heart rhythm called Torsades de Pointes. This risk is highest when starting the drug or increasing the dose.

Certain drugs must NEVER be used with Quinidine due to the risk of fatal heart rhythms or extreme toxicity:

• Thioridazine and Ziprasidone: These antipsychotics also prolong the QT interval; combining them with Quinidine is extremely dangerous.
• Astemizole and Terfenadine: Older antihistamines that can lead to cardiac arrest when combined with Quinidine.
• Ritonavir: This HIV medication significantly increases Quinidine levels to toxic ranges.

• Digoxin

Quinidine must NEVER be used in the following circumstances:

1. 1Complete Heart Block: If the electrical signal cannot pass from the atria to the ventricles at all, Quinidine can suppress the 'backup' rhythm that keeps the heart beating, leading to cardiac arrest.
2. 2History of Quinidine-Induced Thrombocytopenia: If you have ever had a drop in platelets caused by Quinidine, taking it again can cause a life-threatening immune reaction.
3. 3Myasthenia Gravis: Because Quinidine interferes with the transmission of signals between nerves and muscles, it can cause respiratory failure in these patients.
4. 4

Quinidine is classified as FDA Pregnancy Category C. This means that while there are no adequate, well-controlled studies in pregnant women, animal studies have shown potential risks, or the risks are simply unknown. Quinidine does cross the placenta and can reach the fetus. It has been used to treat fetal arrhythmias in specialized cases, but it can also cause uterine contractions. It should only be used during pregnancy if the potential benefit to the mother justifies the potential risk to the fetus. There is no evidence of specific birth defects (teratogenicity), but its use near term may cause neonatal thrombocytopenia.

Quinidine is excreted into breast milk. While the concentration in milk is generally lower than in the mother's blood, the infant's immature liver may not be able to process the drug effectively. A nursing infant could potentially develop cinchonism (tinnitus, vomiting). Most healthcare providers recommend either discontinuing breastfeeding or choosing an alternative medication if the mother must take Quinidine.

Quinidine is not FDA-approved for general use in children. Its use in pediatric patients is typically restricted to the treatment of severe malaria or rare, life-threatening arrhythmias managed by pediatric electrophysiologists. Because children have faster metabolic rates, they may require more frequent dosing, but they are also at higher risk for the gastrointestinal side effects that lead to dehydration.

Quinidine is a Class Ia antiarrhythmic agent. Its primary molecular target is the Nav1.5 voltage-gated sodium channel. By binding to the alpha-subunit of this channel, Quinidine reduces the inward sodium current during Phase 0 of the cardiac action potential. This results in a slower rate of rise of the action potential (Vmax) and slower conduction velocity through the heart's specialized conduction system (His-Purkinje system).

Furthermore, Quinidine blocks several potassium channels, including the IKr (delayed rectifier) channel. This blockade slows down Phase 3 repolarization, which lengthens the total duration of the action potential and increases the effective refractory period (ERP). By making the heart cells 'unresponsive' for a longer period, Quinidine prevents rapid, disorganized electrical signals from triggering arrhythmias.

The clinical effect of Quinidine is directly related to its concentration in the blood. At therapeutic levels (2–6 mcg/mL), it stabilizes the heart rhythm. However, as levels rise, the 'use-dependent' block of sodium channels becomes more pronounced, which can lead to dangerously slow conduction (heart block). The effect on the QT interval is also dose-dependent; the more drug present, the longer the QT interval, and the higher the risk of Torsades de Pointes.