Pharmacokinetic and Metabolic Investigation of Topiramate Disposition in Healthy Subjects in the Absence and in the Presence of Enzyme Induction by Carbamazepine

Britzi, Malka; Perucca, Emilio; Soback, S.; Levy, René H.; Fattore, Cinzia; Crema, Francesca; Gatti, G.; Doose, Dennis R.; Maryanoff, Bruce E.; Bialer, Meir

doi:10.1111/j.0013-9580.2005.55204.x

Cited by 66 publications

(51 citation statements)

References 24 publications

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“…21,23) Enzyme induction by carbamazepine is associated with an approximately 2 to 3-fold increase in topiramate metabolic clearance. 7,10,22,24) It is interesting to note that in some studies in patients taking carbamazepine, topiramate renal clearance was also found to be significantly increased. 10,22) In contrast to carbamazepine, drug interaction with phenobarbital is considered as minor.…”

Section: Discussionmentioning

confidence: 99%

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A Nonlinear Mixed Effects Modelling Analysis of Topiramate Pharmacokinetics in Patients with Epilepsy

Vovk

Jakovljević

Kos

et al. 2010

Biological & Pharmaceutical Bulletin

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Topiramate belongs to the second generation of antiepileptic drugs (AEDs) and has been approved for treatment of adults and children with different kinds of epilepsy as mono or as adjunctive therapy.1,2) The exact mechanism of topiramate action is unknown; however, it is considered that antiepileptic effects are exerted by modulation of voltage-dependent sodium channels, enhancement of g-aminobutyrate (GABA)ergic inhibition on the GABA A receptor, inhibition of carbonic anhydrase isoenzymes, and possibly, through the activity at non-N-methyl-D-aspartate receptors. 1,3,4) The effectiveness of topiramate in adults and children with partial onset and primary generalized seizures was established as initial monotherapy as well as adjunctive treatment. 5)Following oral administration of topiramate, absorption is rapid and almost complete with bioavailability ranging from 81 to 95%. 4,6) Peak plasma concentrations of the drug are reached within 1-4 h after administration. 4,6) Food delays topiramate absorption by approximately 2 h, but the extent of absorption remains unaffected.4) Plasma protein-bound fraction of topiramate varies from 9 to 17%. 4,6) In the dose range 100 to 1200 mg the mean apparent volume of distribution is between 0.6 and 1.0 l/kg. 4,6) In women the volume of distribution is about 50% less than in men, which is attributed to a higher percentage of body fat in women.6) This difference is not considered to be clinically relevant. Over 80% of topiramate is eliminated via the kidneys, predominantly as unchanged drug.6) To date, six trace metabolites formed by glucuronidation, hydroxylation and hydrolysis have been identified in humans. In animal seizure models the metabolites have little or no anticonvulsant activity. 4,6) At steadystate the renal clearance of topiramate is 1.02 l/h 6) and its elimination half-life (t 1/2 ) varies from 20 to 30 h. 1,4) Consequently, the steady-state is being reached in 4 to 8 d.2) Over the dose range 100-800 mg the relationship between topiramate dose and serum concentration is linear in both adults and children. 3,7,8) With the commonly used dosage regimen, serum topiramate concentrations in the range between 16 and 60 mmol/l have been reported.3) A wide range of doses and serum concentrations have been associated with optimal clinical response.3) Topiramate serum concentration was found to correlate with the time to the first seizure, 9) while in the majority of studies no clear relationship between average plasma concentration of topiramate and seizure reduction was found. 6,8,10) Based on these findings, clinical response, rather than blood concentrations is used to guide topiramate dosage adjustments. 1,6) Topiramate pharmacokinetic data mostly come from single dose studies with frequent blood sampling in healthy volunteers as well as from studies with sparse sampling in epileptic patients. However, both types of studies provide little information on inter-and intraindividual variability in pharmacokinetics of topiramate. So far there is no published study with a ...

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Section: Discussionmentioning

confidence: 99%

“…4,7,10,[20][21][22][23][24] Carbamazepine significantly reduces topiramate concentration-to-dose ratio compared to topiramate monotherapy in both children and adults. 21,23) Enzyme induction by carbamazepine is associated with an approximately 2 to 3-fold increase in topiramate metabolic clearance.…”

Section: Discussionmentioning

confidence: 99%

A Nonlinear Mixed Effects Modelling Analysis of Topiramate Pharmacokinetics in Patients with Epilepsy

Vovk

Jakovljević

Kos

et al. 2010

Biological & Pharmaceutical Bulletin

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“…References for drugs whose half-lives are altered in patients receiving liver enzyme inducers: felbamate [36], lamotrigine [37], oxcarbazepine [38], rufinamide [39], tiagabine [40], topiramate [41] and zonisamide [15]. b Half-life increases to 30–90 h during concomitant therapy with valproic acid (enzyme inhibitor).…”

Section: The Challenge Of Establishing Reference Ranges For Aedsmentioning

confidence: 99%

“…Approximately 50% of the absorbed dose is metabolized by the liver, with an increase in metabolism seen in patients concomitantly receiving therapy with classic enzyme inducers. Enzyme inducers can decrease the serum half-life from 20–30 h to approximately 12 h [41,164]. Children generally eliminate topiramate faster than adults [14,165].…”

Section: Topiramatementioning

confidence: 99%

Therapeutic Drug Monitoring of the Newer Anti-Epilepsy Medications

Krasowski

2010

Pharmaceuticals

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In the past twenty years, 14 new antiepileptic drugs have been approved for use in the United States and/or Europe. These drugs are eslicarbazepine acetate, felbamate, gabapentin, lacosamide, lamotrigine, levetiracetam, oxcarbazepine, pregabalin, rufinamide, stiripentol, tiagabine, topiramate, vigabatrin and zonisamide. In general, the clinical utility of therapeutic drug monitoring has not been established in clinical trials for these new anticonvulsants, and clear guidelines for drug monitoring have yet to be defined. The antiepileptic drugs with the strongest justifications for drug monitoring are lamotrigine, oxcarbazepine, stiripentol, and zonisamide. Stiripentol and tiagabine are strongly protein bound and are candidates for free drug monitoring. Therapeutic drug monitoring has lower utility for gabapentin, pregabalin, and vigabatrin. Measurement of salivary drug concentrations has potential utility for therapeutic drug monitoring of lamotrigine, levetiracetam, and topiramate. Therapeutic drug monitoring of the new antiepileptic drugs will be discussed in managing patients with epilepsy.

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“…Approximately 50% of the absorbed dose is metabolized by the liver. Hepatic enzyme inducers can decrease the serum half-life of topiramate from 20-30 hr to approximately 12 hr (Britzi et al, 2005;Sachdeo et al, 1996). Children generally eliminate topiramate faster than adults (Perucca, 2006;Rosenfeld et al, 1999).…”

Section: Topiramatementioning

confidence: 99%

Therapeutic Drug Monitoring of Antiepileptic Medications

Krasowski¹

2011

Novel Treatment of Epilepsy

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Pharmacokinetic and Metabolic Investigation of Topiramate Disposition in Healthy Subjects in the Absence and in the Presence of Enzyme Induction by Carbamazepine

Cited by 66 publications

References 24 publications

A Nonlinear Mixed Effects Modelling Analysis of Topiramate Pharmacokinetics in Patients with Epilepsy

A Nonlinear Mixed Effects Modelling Analysis of Topiramate Pharmacokinetics in Patients with Epilepsy

Therapeutic Drug Monitoring of the Newer Anti-Epilepsy Medications

Therapeutic Drug Monitoring of Antiepileptic Medications

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