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Fluvoxamine

Fluvoxamine (sold as Luvox®, Faverin® and Fevarin®) is a selective serotonin reuptake inhibitor. It is used primarily to treat depression, anxiety and OCD. more...

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Although its effects are similar to other SSRIs, it acts on the body's neurochemistry differently. For this reason, fluvoxamine can be of benefit to patients who experience unusual or limiting side-effects from other antidepressants. Fluvoxamine also appears to cause fewer side-effects than other SSRIs, particularly in relation to loss of sex-drive.

Fluvoxamine has the shortest half-life of all the SSRIs. Its mean serum half-life is 15 hours after a single dose, and 17 to 22 hours after repeated doses.

Fluvoxamine causes many drug-drug interactions due to inhibition of metabolism mediated by several cytochrome P450 oxidases. Examples of substances that have higher serum levels when administered together with fluvoxamine include caffeine, clozapine, olanzapine, tricyclic antidepressants, diazepam, alprazolam, propranolol, warfarin and methadone.

Effective dosage

For depression and anxiety, dosage normally starts at 50 milligrams per day, rising to 100 milligrams after a few days. It may be raised after evaluation of the effects by a doctor.

Fluvoxamine is generally only effective for OCD at 150 milligrams and above, and dosages can reach 300 milligrams or more for some patients.

Historical Relevance

In 1999, fluvoxamine came under great public scrutiny after it was discovered that Eric Harris, one of the two teenaged shooters involved in the Columbine High School massacre, had been taking the drug as treatment for depression. Many immediately pointed fingers at fluvoxamine and its manufacturer Solvay Pharmaceuticals (which sells fluvoxamine under the widely known brandname Luvox), since Solvay's own clinical trials indicated the drug had the propensity to induce "mania" in 4% of the youth who took it. Solvay, while acknowledging the risks inherent in taking an SSRI medication like fluvoxamine, downplayed any role the drug may have had in the killings. The American Psychiatric Association (A.P.A.) took a similar stance; Rodrigo Munoz, M.D., President of the A.P.A., said: "Despite a decade of research, there is little valid evidence to prove a causal relationship between the use of anti-depressant medications and destructive behavior. On the other hand, there is ample evidence that undiagnosed and untreated mental illness exacts a heavy toll on those who suffer from these disorders as well as those around them." It was also pointed out by many that Luvox was often safer than the other SSRI medications available--for example, fluoxetine (Prozac) caused mania in 6% of youth tested on the drug (versus fluvoxamine's 4%). Nonetheless, the reputation of Luvox was irreparably damaged. Sales fell, and Solvay withdrew the medication from the U.S. market in 2002; the company maintains, however, that this move had nothing to do with the safety profile of the fluvoxamine, which they still sell in many countries around the world. In the United States, fluvoxamine can only be purchased generically.

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Small observational study: fluvoxamine not linked to rise in fetal malformation risk
From OB/GYN News, 5/1/04 by Diana Mahoney

MIAMI -- The use of fluvoxamine in pregnancy is not associated with an increased risk of major fetal malformations, according to preliminary results of an ongoing observational study.

Investigators compared the pregnancy outcomes of 46 women taking the selective serotonin reuptake inhibitor to treat depression with those of 46 women taking established nonteratogenic products for the same condition. Anna Sivojelezova reported in a poster presentation at the annual meeting of the American Society for Clinical Pharmacology and Therapeutics.

Fetal survival rates, birth weight, and rates of major malformations did not differ significantly between the two groups. In both groups, "we observed two major fetal malformations," said Ms. Sivojelezova of the Hospital for Sick Children in Toronto.

There were no significant differences in pregnancy outcomes between women who took fluvoxamine (Luvox) throughout pregnancy and those who took it only during the first trimester, she noted.

Because of the study's small sample size, a small increased risk for rare birth defects cannot yet be ruled out, said Ms. Sivojelezova, who, along with her colleagues, is currently recruiting more women for the study.

Currently a Food and Drug Administration category C drug in pregnancy, fluvoxamine is of particular interest because it was the first antidepressant approved by the FDA for obsessive-compulsive disorder, and it is the number one drug prescribed by psychiatrists for this disorder, Ms. Sivojelezova stated.

Because of the high incidence of depression and obsessive-compulsive disorder in women of childbearing age--and because as many as half of all pregnancies are unplanned--information on the safety and efficacy of this drug in pregnancy is necessary to help physicians in pregnancy risk assessment, she stressed.

Ms. Sivojelezova and her associates recruited participants for the study from a list of pregnant women who contacted the hospital's Motherisk Program with questions about the safety of fluvoxamine in pregnancy. Intake coordinators documented participants' medical and obstetric histories, and followed up with a telephone interview after the expected date of delivery. All of the women exposed to fluvoxamine were matched to the control group for disease, age, time of first call to Motherisk, and smoking and drinking habits.

The 4.3% risk of major malformations observed in both the exposed and control groups is within the range for baseline risk (1%-5%) observed in the general population.

BY DIANA MAHONEY

New England Bureau

COPYRIGHT 2004 International Medical News Group
COPYRIGHT 2004 Gale Group

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