Your search keyword '"Perhach JL"' showing total 10 results

1. Coadministration of phenytoin and felbamate: evidence of additional phenytoin dose-reduction requirements based on pharmacokinetics and tolerability with increasing doses of felbamate.

Author

Sachdeo R, Wagner ML, Sachdeo S, Shumaker RC, Lyness WH, Rosenberg A, Ward D, and Perhach JL

Subjects

Adult, Anticonvulsants blood, Anticonvulsants therapeutic use, Dose-Response Relationship, Drug, Drug Administration Schedule, Drug Interactions, Drug Therapy, Combination, Epilepsy blood, Felbamate, Female, Humans, Male, Middle Aged, Phenylcarbamates, Phenytoin blood, Phenytoin therapeutic use, Propylene Glycols blood, Propylene Glycols therapeutic use, Treatment Outcome, Anticonvulsants pharmacokinetics, Epilepsy drug therapy, Phenytoin pharmacokinetics, Propylene Glycols pharmacokinetics

Abstract

Purpose: This open-label study investigated the pharmacokinetic interaction of phenytoin (PHT) and felbamate (FBM)., Methods: Ten subjects with epilepsy receiving PHT monotherapy were administered increasing doses of FBM (1,200, 1,800, 2,400-3,600 mg/day) at 2-week intervals. PHT doses were reduced by 20% on an individual basis when evidence of clinically significant intolerance was present. With intolerance, the PHT dose was reduced before the next incremental FBM dose. Blood samples were analyzed for FBM, PHT, and PHT metabolite 5-(4-hydroxyphenyl)-5-phenylhydantoin (HPPH)., Results: Total PHT plasma concentrations increased with coadministered FBM. PHT Cmax increased from 15.9 microg/ml at baseline to 20.9 microg/ml after 1,200 mg/day FBM and to 26.8 microg/ml after 1,800 mg/day FBM. Four subjects required a 20% PHT dose reduction after 1,800 mg/day FBM and six after the administration of 2,400 mg/day FBM. All subjects required further 20% PHT reductions before 3,600 mg/day FBM. FBM Cmax and AUCT were reduced, and apparent clearance increased compared with data from FBM monotherapy., Conclusions: With the initiation of FBM therapy in subjects receiving PHT, the PHT dosage should be reduced by 20%. Further PHT dose reductions are likely to be necessary if the FBM dose is increased. The requirements for reductions in dose might be predicted by clinical signs of PHT intolerance.

Published

1999

2. Quantification in patient urine samples of felbamate and three metabolites: acid carbamate and two mercapturic acids.

Author

Thompson CD, Barthen MT, Hopper DW, Miller TA, Quigg M, Hudspeth C, Montouris G, Marsh L, Perhach JL, Sofia RD, and Macdonald TL

Subjects

Animals, Carbamates urine, Chromatography, High Pressure Liquid, Epilepsy drug therapy, Epilepsy metabolism, Felbamate, Humans, Mass Spectrometry, Phenylcarbamates, Radioisotope Dilution Technique, Rats, Acetylcysteine urine, Aldehydes urine, Anticonvulsants metabolism, Anticonvulsants urine, Propylene Glycols metabolism, Propylene Glycols urine

Abstract

Purpose: Previously we proposed and provided evidence for the metabolic pathway of felbamate (FBM), which leads to the reactive metabolite, 3-carbamoyl-2-phenylpropion-aldehyde. This aldehyde carbamate was suggested to be the reactive intermediate in the oxidation of 2-phenyl-1,3-propanediol monocarbamate to the major human metabolite 3-carbamoyl-2-phenylpropionic acid. In addition, the aldehyde carbamate was found to undergo spontaneous elimination to 2-phenylpropenal, commonly known as atropaldehyde. Moreover, atropaldehyde was proposed to play a role in the development of toxicity during FBM therapy. Evidence for atropaldehyde formation in vivo was reported with the identification of modified N-acetyl-cysteine conjugates of atropaldehyde in both human and rat urine after FBM administration. Identification of the atropaldehyde-derived mercapturic acids in urine after FBM administration is consistent with the hypothesis that atropaldehyde is formed in vivo and that it reacts with thiol nucleophiles. Based on the hypothesis that the potential for toxicity will correlate to the amount of atropaldehyde formed, we sought to develop an analytic method that would quantify the amount of relevant metabolites excreted in patient urine., Methods: We summarize the results of an LC/MS method used to quantify FBM, 3-carbamoyl-2-phenylpropionic acid and two atropaldehyde-derived mercapturic acids in the patient population., Results: Analysis was performed on 31 patients undergoing FBM therapy. The absolute quantities of FBM and three metabolites were measured., Conclusions: This method demonstrated sufficient precision for the identification of patients exhibiting "abnormal" levels of atropaldehyde conjugates and may hold potential for patient monitoring.

Published

1999

3. Potentially reactive cyclic carbamate metabolite of the antiepileptic drug felbamate produced by human liver tissue in vitro.

Author

Kapetanovic IM, Torchin CD, Thompson CD, Miller TA, McNeilly PJ, Macdonald TL, Kupferberg HJ, Perhach JL, Sofia RD, and Strong JM

Subjects

Biotransformation, Chromatography, High Pressure Liquid, Cytochrome P-450 Enzyme Inhibitors, Enzyme Inhibitors pharmacology, Felbamate, Humans, In Vitro Techniques, Liver enzymology, NAD metabolism, NADP metabolism, Phenylcarbamates, Spectrometry, Mass, Secondary Ion, Anticonvulsants pharmacokinetics, Carbamates metabolism, Liver metabolism, Propylene Glycols pharmacokinetics

Abstract

Felbamate (FBM) is a novel antiepileptic drug that was approved in 1993 for treatment of several forms of epilepsy. After its introduction, toxic reactions (aplastic anemia and hepatotoxicity) associated with its use were reported. It is unknown whether FBM or one of its metabolites is responsible for these idiosyncratic adverse reactions. Although the metabolism of FBM has not been fully characterized, three primary metabolites of FBM have been identified, i.e. 2-hydroxy, p-hydroxy, and monocarbamate metabolites. In addition, the monocarbamate metabolite leads to a carboxylic acid, which is the major metabolite of FBM in humans. Formation of the hydroxylated products of FBM involves cytochrome P450 enzymes, but the enzymes involved in the formation and further metabolism of the monocarbamate have not yet been elucidated. Recently, mercapturate metabolites of FBM have been identified in human urine, and a metabolic scheme involving reactive aldehyde metabolite formation from the monocarbamate metabolite has been proposed. The present study confirmed the formation of the proposed metabolites using human liver tissue in vitro. The aldehyde intermediates were trapped as oxime derivatives, and the cyclic equilibrium product (proposed as a storage and transport form for the aldehydes) was monitored directly by HPLC or GC/MS. Formation of putative toxic aldehyde intermediates and the major carboxylic acid metabolite of FBM was differentially effected with the cofactors NADP+ and NAD+. It is possible that the cofactors may influence the relative metabolism via activation and inactivation pathways.

Published

1998

4. Evaluation of the potential interaction between felbamate and erythromycin in patients with epilepsy.

Author

Sachdeo RC, Narang-Sachdeo S, Montgomery PA, Shumaker RC, Perhach JL, Lyness WH, and Rosenberg A

Subjects

Adult, Anti-Bacterial Agents pharmacology, Anticonvulsants blood, Anticonvulsants therapeutic use, Cross-Over Studies, Drug Interactions, Epilepsy drug therapy, Epilepsy metabolism, Erythromycin pharmacology, Felbamate, Female, Humans, Male, Metabolic Clearance Rate drug effects, Middle Aged, Phenylcarbamates, Propylene Glycols blood, Propylene Glycols therapeutic use, Anti-Bacterial Agents blood, Anticonvulsants pharmacokinetics, Epilepsy blood, Erythromycin blood, Propylene Glycols pharmacokinetics

Abstract

Effects of erythromycin on hepatic CYP450 3A4 isozymes can profoundly influence the metabolism of many therapeutic agents. An open-label, randomized, two-period, crossover study was therefore conducted to evaluate the pharmacokinetics of felbamate before and after a concurrent 10-day regimen (333 mg three times daily) of erythromycin. Patients were receiving either 3,000 or 3,600 mg/day felbamate monotherapy for treatment of epilepsy. Mean dose-normalized values for maximum concentration (Cmax) and area under the concentration-time curve (AUC tau) of felbamate were not statistically different in patients taking felbamate as monotherapy than in patients after erythromycin coadministration. Estimates of time to Cmax (tmax), minimum concentration (Cmin), apparent clearance (Cl/kg), average concentration (Cav), and degree of fluctuation (DFss) were likewise unchanged. The incidence of mild and moderate adverse events increased during coadministration of the two drugs. Because patients with epilepsy can not be treated with erythromycin alone, it could not be determined whether the adverse events were attributable to erythromycin or to the combination of the two drugs. Steady-state pharmacokinetic parameters of felbamate were not influenced by erythromycin coadministration.

Published

1998

5. Pharmacokinetic interactions with felbamate. In vitro-in vivo correlation.

Author

Glue P, Banfield CR, Perhach JL, Mather GG, Racha JK, and Levy RH

Subjects

Anticonvulsants administration & dosage, Anticonvulsants metabolism, Anticonvulsants pharmacology, Area Under Curve, Carbamazepine pharmacokinetics, Cytochrome P-450 Enzyme Inhibitors, Drug Interactions, Enzyme Induction drug effects, Enzyme Inhibitors pharmacokinetics, Enzyme Inhibitors pharmacology, Epilepsy metabolism, Felbamate, Humans, In Vitro Techniques, Isoenzymes antagonists & inhibitors, Neuroprotective Agents administration & dosage, Neuroprotective Agents metabolism, Neuroprotective Agents pharmacology, Phenylcarbamates, Phenytoin pharmacokinetics, Propylene Glycols administration & dosage, Propylene Glycols metabolism, Propylene Glycols pharmacology, Valproic Acid pharmacokinetics, Anticonvulsants pharmacokinetics, Cytochrome P-450 Enzyme System biosynthesis, Isoenzymes biosynthesis, Neuroprotective Agents pharmacokinetics, Propylene Glycols pharmacokinetics

Abstract

This article provides an analysis of the degree of agreement between in vivo interaction studies performed in patients with epilepsy and healthy individuals, and in vitro studies which identified the cytochromes P450 (CYP) inhibited by felbamate and those involved in its metabolism. In vitro studies show that felbamate is a substrate for CYP3A4 and CYP2E1. Compounds which induce CYP3A4 (e.g. carbamazepine, phenytoin and phenobarbital) increase felbamate clearance. However, the CYP3A4 inhibitors gestodene, ethinyl estradiol and erythromycin have little or no effect on felbamate trough plasma concentrations, consistent with the fact that the pathway is relatively minor for felbamate under normal (non-induced) conditions. Felbamate has been shown in vitro to inhibit CYP2C19, which would account for its effect on phenytoin clearance, and it had been postulated that this could be the mechanism underlying the reduced clearance of phenobarbital by felbamate. Although not yet examined in vitro, felbamate appears to induce the activity of CYP3A4, which would account for it reducing plasma concentrations of carbamazepine or the progestin gestodene. Interactions involving felbamate and non-CYP450-mediated metabolic pathways have also been addressed in clinical studies. The reduction in valproic acid (valproate sodium) clearance by felbamate is through the inhibition of beta-oxidation. No clinically relevant pharmacokinetic interactions were noted between felbamate and lamotrigine, clonazepam, vigabatrin, nor the active monohydroxy metabolite of oxcarbazepine. Information on the mechanisms underlying felbamate's drug:drug interaction profile permits predictions to be made concerning the likelihood of interactions with other compounds.

Published

1997

6. Tolerability and pharmacokinetics of monotherapy felbamate doses of 1,200-6,000 mg/day in subjects with epilepsy.

Author

Sachdeo R, Narang-Sachdeo SK, Shumaker RC, Perhach JL, Lyness WH, and Rosenberg A

Subjects

Adolescent, Adult, Anorexia chemically induced, Anticonvulsants adverse effects, Area Under Curve, Dose-Response Relationship, Drug, Drug Administration Schedule, Epilepsy blood, Felbamate, Female, Headache chemically induced, Humans, Middle Aged, Nausea chemically induced, Phenylcarbamates, Propylene Glycols adverse effects, Treatment Outcome, Anticonvulsants administration & dosage, Anticonvulsants pharmacokinetics, Epilepsy drug therapy, Propylene Glycols administration & dosage, Propylene Glycols pharmacokinetics

Abstract

Purpose: Felbamate (FBM) pharmacokinetic parameters, safety and tolerability in the dose range of 1,200-6,000 mg/day were assessed in two open-label studies with similar designs., Methods: In study A, newly diagnosed subjects with epilepsy receiving FBM monotherapy at a starting dose of 1,200 mg/day (400 mg/three times daily, t.i.d.) and increased 1,200 mg/day, if tolerated, at 14-day intervals to 3,600 mg/day were investigated. In study B, epilepsy subjects with prior FBM monotherapy exposure received ascending FBM doses in five consecutive 14-day periods with a starting dose of 3,600 mg/day (1,200 mg t.i.d.) FBM. In each successive period, if FBM was well tolerated, the dose was increased by 600 mg/day to a maximum of 6,000 mg/day (2,000 mg t.i.d.)., Results: The pharmacokinetic parameter estimates maximum observed concentration (Cmax), area under the concentration-time curve (AUCtau) Ctrough, and Cav showed a linear dependence to dose above the 1,200-6,000 mg/day FBM dose range (F-tests; p < 0.0001) with apparent clearance (Cl/kg) and Tmax (time to Cmax) independent of dose. When AUCtau, Cmax and Ctrough were adjusted for dose, there were no significant differences between the dosing periods., Conclusions: The data establish that plasma concentrations of FBM are linear with respect to dose to 6,000 mg/day. In addition, FBM was safely administered at these doses for periods as long as 14 days to epileptic subjects with prior exposure to FBM. FBM-naive subjects appeared to report more adverse experiences (generally of mild to moderate severity) than did subjects with prior FBM exposure.

Published

1997

7. The effect of age on the apparent clearance of felbamate: a retrospective analysis using nonlinear mixed-effects modeling.

Author

Banfield CR, Zhu GR, Jen JF, Jensen PK, Schumaker RC, Perhach JL, Affrime MB, and Glue P

Subjects

Adolescent, Adult, Aged, Bayes Theorem, Body Weight physiology, Child, Child, Preschool, Drug Interactions, Felbamate, Female, Humans, Male, Middle Aged, Models, Biological, Phenylcarbamates, Population, Regression Analysis, Retrospective Studies, Aging metabolism, Anticonvulsants pharmacokinetics, Propylene Glycols pharmacokinetics

Abstract

The effects of age on felbamate apparent clearance were examined through a retrospective analysis of plasma concentration data from 700 pediatric and adult epileptic patients (age range, 2-74 years) enrolled in six clinical studies. Patients received felbamate as monotherapy or in combination with either the antiepileptic drugs (AEDs) carbamazepine (CBZ), phenytoin (PHT), or valproate (VPA). Data were analyzed using a nonlinear mixed-effects pharmacostatistical modeling technique (NONMEM). Factors in the model included age, body weight, and concomitant AEDs. Apparent clearance was highest in the very young and decreased during the early teenage years, with minimal changes observed beyond 13 years. Mean apparent clearance values were approximately 40% higher in children (2-12 years) compared with those in adults (13-65 years). This pattern and its magnitude were consistent whether felbamate was administered alone or coadministered with CBZ, PHT, or VPA. The increase in clearance is minimal compared with other AEDs including PHT, CBZ, and phenobarbital. Enzyme-inducing AEDs (CBZ and PHT) increased felbamate apparent clearance by 32-38% relative to monotherapy, whereas coadministration with VPA had a minimal effect on felbamate apparent clearance. Dose/concentration linearity was observed at all ages during mono- or polytherapy. These findings suggest that felbamate dosing should be relatively uncomplicated in children relative to that in adults.

Published

1996

8. Comment: warfarin-felbamate interaction.

Author

Glue P, Banfield CR, Colucci RD, and Perhach JL

Subjects

Drug Interactions, Felbamate, Humans, Phenylcarbamates, Stereoisomerism, Anticonvulsants adverse effects, Propylene Glycols adverse effects, Warfarin adverse effects

Published

1994

9. The effect of felbamate on valproic acid disposition.

Author

Wagner ML, Graves NM, Leppik IE, Remmel RP, Shumaker RC, Ward DL, and Perhach JL

Subjects

Adult, Cross-Over Studies, Drug Therapy, Combination, Epilepsy drug therapy, Felbamate, Female, Humans, Male, Phenylcarbamates, Propylene Glycols administration & dosage, Propylene Glycols adverse effects, Propylene Glycols blood, Propylene Glycols pharmacokinetics, Protein Binding, Valproic Acid administration & dosage, Valproic Acid adverse effects, Valproic Acid blood, Epilepsy metabolism, Propylene Glycols pharmacology, Valproic Acid pharmacokinetics

Abstract

Introduction: Felbamate is a new antiepileptic drug approved for partial and secondarily generalized seizures., Design: Subjects with epilepsy (three men and seven women; age range, 20 to 39 years; weight range, 53 to 88 kg) who were previously stabilized with valproic acid, 9.5 to 31.7 mg/kg/day, received both 600 and 1200 mg felbamate twice a day in an open-label, randomized, crossover study., Results: Coadministration of 1200 or 2400 mg felbamate increased the mean valproic acid area under the curve (from 802.2 to 1025.4 and 1235.9 mg/hr/ml, respectively), peak concentrations (from 86.1 to 115.1 and 133.4 mg/ml, respectively), and average steady-state concentrations (from 66.9 to 85.5 and 103.0 mg/ml, respectively). No changes were observed in valproic acid time to peak concentration or protein binding. Average steady-state felbamate concentrations were 34.7 mg/ml for 600 mg administered twice daily and 61.2 mg/ml for 1200 mg administered twice daily., Conclusion: When felbamate is added to a regimen of valproic acid, valproic acid doses may require reduction because coadministration of felbamate decreased steady-state valproic acid clearance (28% and 54%, respectively; p < 0.01).

Published

1994

10. Felbamate.

Author

Sofia RD, Kramer L, Perhach JL, and Rosenberg A

Subjects

Administration, Oral, Animals, Anticonvulsants adverse effects, Anticonvulsants pharmacokinetics, Dose-Response Relationship, Drug, Drugs, Investigational adverse effects, Drugs, Investigational pharmacokinetics, Electroencephalography drug effects, Epilepsy blood, Felbamate, Humans, Phenylcarbamates, Propylene Glycols adverse effects, Propylene Glycols pharmacokinetics, Rats, Anticonvulsants therapeutic use, Drugs, Investigational therapeutic use, Epilepsy drug therapy, Propylene Glycols therapeutic use

Published

1991