Domperidone chemical structure
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Domperidone

Domperidone (Motilium®) is an antidopaminergic drug used orally or intravenously, generally to suppress nausea and vomiting. It has also been used to stimulate lactation. more...

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Uses

Gastrointestinal problems

Domperidone is used, together with metoclopramide, cyclizine, and 5HT3 receptor antagonists (such as granisetron) in the treatment of nausea and vomiting. It is useful in patients with Parkinson's disease because, unlike metoclopramide, domperidone does not cross the blood-brain barrier. Domperidone is also prescribed for the treatment of gastroparesis, a stomach motility condition.

Lactation

The hormone prolactin stimulates lactation in humans, and its release is inhibited by the dopamine secreted by the hypothalamus. Domperidone, by acting as an anti-dopaminergic, results in increased prolactin secretion, and thus promotes lactation.

Although it has never been officially approved for use in the United States, domperidone is widely purchased from pharmacies in other countries for this purpose.

Problems

In June 2004, the United States' main regulation agency, the Food and Drug Administration (FDA) issued a letter warning women not to take domperidone, citing unknown risks to parents and infants, and warned pharmacies that domestic sale was illegal, and that import shipments from other countries would be searched and seized. Individual incidents of problems with the drug include cardiac arrest and arrhythmia, complications with other medications, as well as complications with improper intravenous use.

It has been widely speculated that this action by the FDA is related to increasing drug importation from countries such as Canada. However, organisations such as the American Association of Pediatrics have endorsed the FDA action.

Yet prominent doctors and pharmacists have rejected the FDA's reasoning and still promote domperidone's use in increasing milk supply. Such doctors and pharmacists are confident the drug is safe in the doses given for this purpose. The American Academy of Pediatrics considers domperidone "usually compatible with breastfeeding."

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Drug-induced prolongation of the QT interval
From American Family Physician, 1/1/05 by Bill Zepf

The most common reason for removing a prescription drug from the U.S. market in the past decade has been prolongation of the QT interval. There is an increased risk for the development of torsades de pointes, a potentially fatal arrhythmia, when the QT interval is prolonged. Roden reviewed the drugs most commonly implicated in QT prolongation and the clinical factors that increase the risk of torsades de pointes.

Medication-induced QT prolongation was first recognized with the use of quinidine in the 1920s. Roden lists other drugs that also are implicated in prolongation of the QT interval and may cause torsades de pointes (Table 1). Use of these medications, especially when a congenital QT prolongation syndrome or other clinical risk factor is present, increases the chance that torsades de pointes may develop (Table 2). Because the risk of torsades de pointes is sufficiently high at typical clinical dosages of sotalol, dofetilide, and ibutilide, the review author recommends inhospital cardiac monitoring when therapy with these agents is initiated.

The risk of torsades de pointes is not related linearly to the degree of QT prolongation, although any drug that prolongs the QT interval beyond 500 msec is thought to confer an elevated risk. Heart rate exerts an important effect on the risk for associated torsades de pointes, with a greater propensity for developing the arrhythmia when bradycardia is present.

QT prolongation occurs when a drug or congenital syndrome affects ion channels in cardiac cells and leads to prolongation of the action potential during depolarization. This step may lead to a reduced reserve for normal repolarization, which then increases the risk of developing torsades de pointes. However, these known links do not explain completely the risk of torsades de pointes. Amiodarone often causes QT prolongation beyond 500 msec, yet rarely causes torsades de pointes. Terfenadine was removed from the market because of associated episodes of torsades de pointes, yet therapeutic dosages only extended the QT interval by 6 msec. The degree of QT prolongation caused by a given medication can be influenced by the concomitant use of other agents that inhibit drug elimination. Examples cited by Roden include erythromycin, clarithromycin, ketoconazole, itraconazole, amiodarone, quinidine, and a number of antidepressants and antiretrovirals.

The author concludes that when physicians need to use a medication known to have the effect of prolonging the QT interval, a review of other risk factors that may increase the likelihood that torsades de pointes will develop is recommended. Therefore, an elderly woman with heart failure who also takes medications that might indirectly lead to increased risk (e.g., diuretic use causing hypokalemia) would be a particularly risky candidate for use of a drug that prolongs the QT interval. Close clinical and electrocardiographic monitoring would be prudent during treatment.

Roden DM. Drug-induced prolongation of the QT interval. N Engl J Med March 4, 2004;350:1013-22.

COPYRIGHT 2005 American Academy of Family Physicians
COPYRIGHT 2005 Gale Group

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