Topiramate chemical structure
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Topiramate

Topiramate (brand name: Topamax®) is an anticonvulsant drug produced by Ortho-McNeil, a division of Johnson & Johnson. It is used to treat epilepsy in both children and adults. In children it is also indicated for treatment of Lennox-Gastaut syndrome (a disorder that causes seizures and developmental delays). It is also FDA approved for, and now most frequently prescribed for, the prevention of migraines. It has been used by psychiatrists to treat bipolar disorder, although it is not FDA approved for this purpose and such use is somewhat controversial. more...

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This drug has been investigated for use in treatment of obesity, especially to aid in the reduction of binge eating, and also as a possible treatment for alcoholism. However, these uses are not actively promoted by the manufacturer, and like its use for bipolar disorder, are "off-label" uses. The drug is also used in clinical trials to treat Post Traumatic Stress Disorder. A pilot study suggests that Topiramate is possibly effective against infantile spasm.

Pharmacodynamics

Chemically, Topiramate is a sulfamate-substituted monosaccharide, related to fructose, a rather unusual chemical structure for an anticonvulsant. Topiramate is quickly absorbed after oral use. Most of the drug (70%) is excreted in the urine as unchanged drug. The remainder is extensively metabolized by hydroxylation, hydrolysis, and glucuronidation. Six metabolites have been identified in humans, none of which constitutes more than 5% of an administered dose. Topiramate enhances GABA-activated chloride channels. In addition, Topiramate inhibits excitatory neurotransmission, through actions on kainate and AMPA receptors. There is evidence that Topiramate has a specific effect on GluR5 kainate receptors. It is also an inhibitor of carbonic anhydrase, particular subtypes II and IV, but this action is weak and unlikely to be related to its anticonvulsant actions, but may account for the bad taste and the development of renal stones seen during treatment. Its possible effect as a mood stabilizer seems to occur before anticonvulsant qualities at lower dosages. Topiramate inhibits maximal electroshock and pentylenetetrazol-induced seizures as well as partial and secundarily generalized tonic-clonic seizures in the kindling model, findings predective of a broad spectrum of antiseizure activities clinically.

Side effects

The most common side effects include a change in taste (carbonated beverages, especially diet sodas and beer, taste particularly bad) and feelings of pins and needles in the head and extremities. Less common side effects include cognitive deficiency (particularly word-finding difficulty); grogginess; lethargy; renal stones, impairment of fine motor skills; vision abnormality and transient or permanent vision loss (see below for FDA warning); weight loss; breast pain; abdominal pain; menstrual disorder; taste changes; pharyngitis; sinusitis; diplopia; rash; leukopenia; fatigue; dizziness; insomnia; anxiety; depression; paresthesia; diarrhea; nausea; dyspepsia; constipation; dry-mouth; dysmenorrhea.

Rarely, the inhibition of carbonic anhydrase may be strong enough to cause metabolic acidosis of clinical importance.

The side-effects most frequently leading to discontinuation of therapy with topiramate were :

Read more at Wikipedia.org


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A trial of topiramate for migraine prophylaxis
From American Family Physician, 10/15/04 by Caroline Wellbery

Migraine headache is a common and disabling disorder. Less than one third of treated patients report consistently effective results from their current pharmacologic regimens, and many patients do not seek treatment. Habitual overuse of acute medications, including triptans, ergots, and analgesics, can lead to chronic daily headache. Prophylaxis may reduce migraine frequency and prevent dosage escalation of acute therapies. Brandes and colleagues investigated whether an antiepileptic medication, topiramate, would be effective in preventing migraines.

Patients who were 12 to 65 years of age and had three to 12 migraines a month were included in the study. Patients who had failed more than two previous prophylactic medication trials were excluded, as were patients taking beta blockers, antidepressants, antiepileptic drugs, calcium channel blockers, and other medications that might confound the trial results. After a washout period of 14 days, followed by a 28-day baseline period, eligible patients were randomized to treatment with placebo or topiramate in a dosage of 50 mg per day, 100 mg per day, or 200 mg per day, with dosages titrated upward in 25-mg weekly increments to the target dosage. After an 18-week maintenance period, patients were eligible to continue an openlabel extension after a blinded seven-week transition.

Patients kept a headache and rescue medication diary. The primary efficacy measure was a comparison of the reduction in migraine frequency from baseline. Other measures included the proportion of patients responding to treatment; a change in the number of monthly migraine days, severity, and duration; and a change in number of days requiring rescue medication. Of the 483 patients enrolled, 63 in the placebo group completed the trial, as did 59 in the 50-mg topiramate group, 63 in the 100-mg group, and 70 in the 200-mg group, for a total of 255 patients completing the study. The mean monthly migraine frequency in all patients at baseline was 5.5, and the mean monthly number of migraine days was 6.5. In all groups, 15 to 24 percent of patients were taking prophylactic medication in the three months before the prospective baseline phase.

Topiramate therapy was associated with a greater reduction in monthly migraine frequency than was achieved with placebo. When compared with placebo, the difference was statistically significant in patients receiving 100 mg and 200 mg of topiramate, but not in those receiving 50 mg. Among placebo patients, headaches were reduced from 5.6 per month to 4.5; in the 100-mg topiramate group, headaches were reduced from 5.8 to 3.5 per month, and from 5.1 to 3.0 in patients receiving 200 mg of topiramate per day. The difference at these dosages occurred by one month of treatment and remained statistically significant for the duration of the trial.

A significantly larger proportion of patients in all topiramate groups had at least a 50 percent reduction in monthly migraine frequency compared with the placebo group. Topiramate in the higher dosages also was associated with a statistically significant reduction in mean monthly number of migraine days and number of days requiring the use of rescue medication. Adverse events associated with topiramate occurred in 10 percent or more of patients, leading to discontinuation by some participants.

The authors conclude that, compared with placebo, topiramate at dosages of 100 or 200 mg per day significantly reduces migraine frequency and the number of days requiring rescue medications. Because of adverse events, slow upward titration may enhance tolerability. The study results also suggest that, for migraine prophylaxis, topiramate is at least as effective as other preventive agents, including propranolol, amitriptyline, and valproate.

CAROLINE WELLBERY, M.D.

Brandes JL, et al., for the MIGR-002 Study Group. Topiramate for migraine prevention. A randomized controlled trial. JAMA February 25, 2004;291:965-73.

COPYRIGHT 2004 American Academy of Family Physicians
COPYRIGHT 2004 Gale Group

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