© 2012 Direct One Communications, Inc. All rights reserved. 1 Emerging Developments in Antiepileptic Drug Therapy Jeffrey D. Kennedy, MD Northwestern University.

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Presentation transcript:

© 2012 Direct One Communications, Inc. All rights reserved. 1 Emerging Developments in Antiepileptic Drug Therapy Jeffrey D. Kennedy, MD Northwestern University Feinberg School of Medicine, Chicago, Illinois A REPORT FROM THE 64 th ANNUAL MEETING OF THE AMERICAN ACADEMY OF NEUROLOGY

© 2012 Direct One Communications, Inc. All rights reserved. 2 Over the past several decades, exciting developments in our understanding and management of epilepsy have included: Progress in Treating Epilepsy Renewed enthusiasm for surgery. Trials of new therapeutic neurostimulation devices. Approval of several new antiepileptic drugs (AEDs).

© 2012 Direct One Communications, Inc. All rights reserved. 3 And Lack of Progress As Well… These advances have so far produced little improvement in patients achieving freedom from their seizures. 1,2 Up to 40% of patients with epilepsy remain refractory to treatment with AEDs. 3 At best, current surgical treatment offers long-term seizure freedom in 60%–70% of selected ideal patients. 4 Surgery is not an option for many other individuals, and neurostimulation offers little more than a palliative option.

© 2012 Direct One Communications, Inc. All rights reserved. 4 Current Research Directions 1,5,6 Identifying novel therapeutic targets Defining mechanisms of action of novel AEDs Developing new preclinical evaluation methods to pinpoint more effective/safer treatments Reevaluating current therapies in special patient populations Improving the design and efficacy of neurostimulation devices Treating comorbidities associated with epilepsy Refining clinical trial designs

© 2012 Direct One Communications, Inc. All rights reserved. 5 Zonisamide

© 2012 Direct One Communications, Inc. All rights reserved. 6 Zonisamide Zonisamide was approved by the FDA in 2000 for the adjunctive treatment of partial seizures in adults. Its mechanisms of action 7 include: » Acting as a sodium-channel antagonist » Reducing inward T-type calcium-channel currents » Inhibiting neurotransmitters primarily by affecting gamma-aminobutyric acid, serotonin, and dopamine levels It is essentially devoid of clinically significant interactions with other AEDs, oral contraceptives, and other classes of therapeutic agents. 8

© 2012 Direct One Communications, Inc. All rights reserved. 7 CATZ Trial: Patients and Methods This recently completed phase III trial assessed the efficacy and safety of zonisamide in 207 patients with partial seizures who were 6–17 years of age. 9 Patients were being treated with one or two AEDs at baseline. Zonisamide (n = 107) was titrated from 1 mg/kg/d to 8 mg/kg/d over 8 weeks. » Patients were maintained on that dosage for 12 weeks and either continued using 8 mg/kg/d as part of an extension study or were gradually withdrawn from zonisamide therapy. The remaining 100 patients received placebo.

© 2012 Direct One Communications, Inc. All rights reserved. 8 Endpoints were: A  50% reduction in frequency of seizures Median percent change from baseline in 28-day seizure frequency during the 12-week maintenance period and the entire double-blind period (ie, titration plus maintenance) The study was completed by: 93 patients given zonisamide (87%) 90 patients given placebo (90%) CATZ Trial: Patients and Methods

© 2012 Direct One Communications, Inc. All rights reserved. 9 CATZ Trial: Efficacy A  50% reduction in seizure frequency was achieved in 50.5% of patients given 8 mg/kg/d of zonisamide and 31.0% of those given placebo. The median percent change in baseline 28-day seizure frequency was: » –50.0 % for zonisamide vs –24.5% for placebo during the maintenance phase (between-group difference, 25.2%) » –42.2% for zonisamide vs –20.4% for placebo during the double-blind period (between-group difference, 25.3%)

© 2012 Direct One Communications, Inc. All rights reserved. 10 CATZ Trial: Safety and Tolerability The most common adverse reactions (headache, decreased appetite, nasopharyngitis, and upper abdominal pain) were reported in: » 55.1% of patients receiving zonisamide » 50.0% of those given placebo Events significantly more associated with zonisamide than placebo included: » Decreased appetite » Weight loss » Somnolence » Vomiting » Diarrhea

© 2012 Direct One Communications, Inc. All rights reserved. 11 Severe adverse events and those leading to withdrawal from the study occurred more often in the placebo group than in patients taking zonisamide. Serious adverse events were seen in four patients given zonisamide (3.7%) and two using placebo (2.0%). CATZ Trial: Safety and Tolerability

© 2012 Direct One Communications, Inc. All rights reserved. 12 CATZ Trial: Conclusions Zonisamide is an effective adjunctive treatment for partial-onset seizures in children  6 years of age when compared with placebo. Use of zonisamide in this pediatric population was not associated with serious or new adverse effects or safety concerns.

© 2012 Direct One Communications, Inc. All rights reserved. 13 Perampanel

© 2012 Direct One Communications, Inc. All rights reserved. 14 Perampanel Perampanel is a first-in-class, highly selective, noncompetitive  -amino-3-hydroxy-5-methyl-4- isoxazolepropionic acid (AMPA)-type glutamate receptor antagonist being developed for adjunctive treatment of patients with partial-onset seizures. Recent studies have focused on AMPA receptors, which 10 : » Transmit the majority of fast glutaminergic signaling » May play a central role in seizure generation and spread Perampanel is currently under review by the FDA.

© 2012 Direct One Communications, Inc. All rights reserved. 15 Global Phase III Studies of Perampanel Perampanel effectively reduced seizure frequency when given as adjunctive therapy to patients with refractory partial-onset epilepsy in three global, multicenter, double-blind, parallel-group trials 11–15 : » Study 304 » Study 305 » Study 306 These studies were performed in three phases: » Prerandomization (baseline period) » A double-blind phase » A follow-up period

© 2012 Direct One Communications, Inc. All rights reserved. 16 Global Phase III Studies of Perampanel: Patients and Methods A total of 1,478 patients (age  12 years) with uncontrolled focal or partial-onset seizures while taking up to three AEDs were randomized to receive adjunctive therapy with either: » 8 or 12 mg/d of perampanel or placebo (studies 304 and 305) over 6 weeks or » 2, 4, or 8 mg/d of perampanel or placebo (study 306) over 6 weeks Dosage was titrated upward by 2 mg/wk until the target dose was reached. Patients then continued on maintenance therapy for 13 weeks.

© 2012 Direct One Communications, Inc. All rights reserved. 17 Patients were excluded from the studies if they had: » Generalized epilepsy or » Lennox-Gastaut syndrome or » A history of status epilepticus within the previous year Seizures were recorded daily in a patient diary and normalized to 28 days for analysis. Global Phase III Studies of Perampanel: Patients and Methods

© 2012 Direct One Communications, Inc. All rights reserved. 18 Global Phase III Studies of Perampanel: Response Rate and Seizure Freedom 11 To determine the dose-response rate, 50%, 75%, and 100% responder rates were evaluated in patients given 2, 4, 8, or 12 mg/d of perampanel. Data were pooled from the three phase III trials with a 6-week titration period and 13-week maintenance period (n = 442). The median 28-day baseline seizure rate varied from 10.2 to 18.9 across the three studies. Central and South American patients were excluded due to a regional effect that resulted in a high placebo response.

© 2012 Direct One Communications, Inc. All rights reserved. 19 Global Phase III Studies of Perampanel: Response Rate and Seizure Freedom 11 Use of 4–12 mg/d of perampanel significantly increased 50% and 75% responder rates in a dose- dependent manner. A trend toward seizure freedom with increasing perampanel exposure was observed.

© 2012 Direct One Communications, Inc. All rights reserved. 20 Global Phase III Studies of Perampanel: Time to Recurrence 12 A novel study design was used to measure median and individualized “time to event” to: » Reduce baseline variability » Allow patients to complete studies with less drug exposure Data were pooled from all three phase III studies. Patients from Central and South America were excluded.

© 2012 Direct One Communications, Inc. All rights reserved. 21 Global Phase III Studies of Perampanel: Time to Recurrence 12 Endpoints were median times to 1 st, 3 rd, 6 th, 9 th, and 12 th seizure events. The individualized temporal endpoint was the median time for patients to reach their baseline 28- day seizure rate (N th seizure). Adjunctive therapy with perampanel prolonged: » Median times to baseline 28-day seizure rate » Median time to next seizure over baseline » Median times to 6 th, 9 th, and 12 th seizure events

© 2012 Direct One Communications, Inc. All rights reserved. 22 Global Phase III Studies of Perampanel: Time to Recurrence 12

© 2012 Direct One Communications, Inc. All rights reserved. 23 Global Phase III Studies of Perampanel: Time to Recurrence 12 Adjunctive treatment of partial-onset seizures with 4–12 mg/d of perampanel effectively prolonged the 28-day seizure rate and time to next seizure. The lack of seizure-rate prolongation with 12 mg/d likely was due to most patients experiencing a 12 th seizure before receiving the full 12-mg daily dose. The results supported the use of individualized “time to event” assessments in future studies. Adequate evaluation of later or higher drug exposure may be better reflected by endpoints involving longer titration periods and/or a higher frequency of seizures at baseline.

© 2012 Direct One Communications, Inc. All rights reserved. 24 Global Phase III Studies of Perampanel: Efficacy with Concomitant AED Therapy 13 The effect of concomitant AED administration on perampanel efficacy was analyzed via assessment of seizure frequency and responder rate. A total of 1,478 pooled phase II trial participants were included. After randomization: » 180 patients were given 2 mg/d of perampanel. » 172 patients were given 4 mg/d of perampanel. » 431 patients were given 8 mg/d of perampanel. » 254 patients were given 12 mg/d of perampanel. » 441 patients were given placebo.

© 2012 Direct One Communications, Inc. All rights reserved. 25 Global Phase III Studies of Perampanel: Efficacy with Concomitant AED Therapy 13 Endpoints were the median percent change in 28-day seizure frequency and 50% responder rate. Patients used an average of 2.2 concomitant AEDs, most commonly: » Carbamazepine (n = 491) » Valproate (n = 478) » Lamotrigine (n = 457) » Levetiracetam (n = 435)

© 2012 Direct One Communications, Inc. All rights reserved. 26 Global Phase III Studies of Perampanel: Efficacy with Concomitant AED Therapy 13

© 2012 Direct One Communications, Inc. All rights reserved. 27 In summary, 4–12 mg/d of perampanel is an effective adjuvant therapy for reducing seizure frequency and increasing responder rates in patients with partial-onset seizures due to epilepsy. The efficacy of perampanel is not influenced by concomitant use of other AEDs. Global Phase III Studies of Perampanel: Efficacy with Concomitant AED Therapy 13

© 2012 Direct One Communications, Inc. All rights reserved. 28 The pharmacokinetic and pharmacodynamic effects of perampanel as they related to demographic factors and concomitant AED administration were studied. An analysis of predicted exposure/efficacy with the last dose achieved in a model also was performed. Of the 1,478 participants in the three phase III trials: » A total of 1,109 patients were included in the pooled pharmacokinetic/pharmacodynamic study. » In all, 770 patients were included in the pharmacokinetic study alone, including 745 in the last-dose analysis. Global Phase III Studies of Perampanel: Efficacy with Concomitant AED Therapy 14

© 2012 Direct One Communications, Inc. All rights reserved. 29 Blood samples taken at baseline, during the double- blind treatment phases, maintenance therapy periods, and at the end of the follow-up phases or upon discontinuation of perampanel therapy were compared. Perampanel concentrations in the blood samples were determined via liquid chromatography and mass spectroscopy. Global Phase III Studies of Perampanel: Efficacy with Concomitant AED Therapy 14

© 2012 Direct One Communications, Inc. All rights reserved. 30 Twelve concomitant AEDs were used by at least 50 patients in the pharmacokinetic/pharmacodynamic population analysis. Approximately 1% of patients were prescribed at least one perampanel inducer. Mean plasma perampanel concentrations remained linear over the dose range, regardless of concomitant AED therapy. Seizure frequency decreased and 50% responder rate increased in a linear fashion with increasing perampanel serum level at steady state, regardless of the presence of a concomitant perampanel inducer. Global Phase III Studies of Perampanel: Efficacy with Concomitant AED Therapy 14

© 2012 Direct One Communications, Inc. All rights reserved. 31 Adverse effects increased with increasing exposure to perampanel and were not affected by demographic factors or the concomitant use of other AEDs, including perampanel inducers. No change in appetite or headaches related to perampanel concentration was observed. Age, gender, body mass, and race had no affect on the probability of response to perampanel or occurrence of adverse effects. Global Phase III Studies of Perampanel: Efficacy with Concomitant AED Therapy 14

© 2012 Direct One Communications, Inc. All rights reserved. 32 Global Phase III Studies of Perampanel: Dose-Response Analysis 15 Seizure frequency over 28 days and 50% responder rates were assessed in patients enrolled in the three pooled phase III trials and an open-label extension study (OLE 307). » The study included 209 patients who completed one of the double-blind phase III studies on 8 mg/d of perampanel to start and then were titrated upward to 12 mg/d during the conversion period of the OLE study. Data on patients randomized to receive 12 mg/d of perampanel by the conversion period were assessed. Central and South American patients were excluded from the analysis due to a regional placebo effect.

© 2012 Direct One Communications, Inc. All rights reserved. 33 Global Phase III Studies of Perampanel: Dose-Response Analysis 15 Improved perampanel efficacy, as judged by a greater reduction in 28-day seizure frequency and higher 50% responder rate, may be achieved by increasing the dosage of perampanel from 8 mg/d to 12 mg/d.

© 2012 Direct One Communications, Inc. All rights reserved. 34 Summary Both zonisamide and perampanel have demonstrated: Promising efficacy in pediatric and adult patients, respectively, with refractory partial-onset seizures. The potential to improve the current level of AED efficacy. The potential to provide new options for the treatment of epilepsy in these populations.

© 2012 Direct One Communications, Inc. All rights reserved. 35 References 1.Löscher W, Schmidt D. Modern antiepileptic drug development has failed to deliver: ways out of the current dilemma. Epilepsia. 2011;52:657– Beyenburg S, Stavem K, Schmidt D. Placebo-corrected efficacy of modern antiepileptic drugs for refractory epilepsy: systematic review and meta-analysis. Epilepsia. 2010;51:7–26. 3.Kwan P, Brodie MJ. Early identification of refractory epilepsy. N Engl J Med. 2000;342:314– Tellez-Zenteno JF, Dhar R, Wiebe S. Long-term seizure outcomes following epilepsy surgery: a systematic review and meta-analysis. Brain. 2005;128:1188– Galanopoulou AS, Buckmaster PS, Staley KJ, et al. Identification of new epilepsy treatments: issues in preclinical methodology. American Epilepsy Society Basic Science Committee; The International League Against Epilepsy Working Group on Recommendations for Preclinical Epilepsy Drug Discovery. Epilepsia. 2012;53:571– Loscher W. Critical review of current animal models of seizures and epilepsy used in the discovery and development of new antiepileptic drugs. Seizure. 2011;20:359– Leppik IE. Zonisamide: chemistry, mechanism of action, and pharmacokinetics. Seizure. 2004;13:S5–S9. 8.Brodie MJ, Duncan R, Vespignani H, Solyom A, Bitenskyy V, Lucas C. Dose-dependent safety and efficacy of zonisamide: a randomized, double-blind, placebo-controlled study in patients with refractory partial seizures. Epilepsia. 2005;46:31–41. 9.Rosati A, Segieth J, Giorgi L, Guerrini R. Results from the CATZ study: a phase III, double-blind, randomized, placebo-controlled trial to assess the efficacy and safety of adjunctive zonisamide in pediatric patients with partial-onset seizures. Neurology. 2012;78:P Rogawski M. Revisiting AMPA receptors as an antiepileptic drug target. Epilepsy Curr. 2011;11:56–63.

© 2012 Direct One Communications, Inc. All rights reserved. 36 References 11.Krauss G, Perucca E, Brodie M, et al. Pooled analysis of responder rates and seizure freedom from phase III clinical trials of adjunctive perampanel, a selective, non-competitive AMPA receptor antagonist. Neurology. 2012;78:P Laurenza A, French J, Gil-Nagel A, et al. Perampanel, a selective, non-competitive AMPA receptor antagonist, prolongs time to seizure recurrence in patients with epilepsy: results of pooled phase III clinical trial data. Neurology. 2012;78:S French J, Ben-Menachem E, Brodie M, et al. Efficacy of adjunctive perampanel in phase III clinical trials: subanalysis of change in seizure frequency and responder rates by concomitant antiepileptic drug use. Neurology. 2012;78:S Hussein Z, Ferry J, Krauss G, Squillacote D, Laurenza A. Demographic factors and concomitant antiepileptic drugs have no effect on the pharmacodynamics of perampanel. Neurology. 2012;78:P Kramer L, Perucca E, Ben-Menachem E, et al. Perampanel, a selective, noncompetitive AMPA receptor antagonist as adjunctive therapy in patients with refractory partial-onset seizures: a dose response analysis from phase III studies. Neurology. 2012;78:P