Safety and Pharmacokinetics Study of E2007 to Treat Partial and Generalised Seizures in People With Epilepsy

Eisai Co., Ltd.18 enrolled

Overview

The objectives of this study were to assess the tolerability and safety of E2007 in patients with refractory partial or generalised seizures and to assess the pharmacokinetics of E2007 in epileptic patients receiving at least one concomitant anti-epileptic drug.

Study Type

INTERVENTIONAL

Allocation

RANDOMIZED

Purpose

TREATMENT

Masking

DOUBLE

Enrollment

Conditions

Epilepsy

Interventions

E2007DRUG

1 mg of E2007 was administered by mouth once daily.

E2007DRUG

2 mg of E2007 was administered by mouth once daily.

PlaceboDRUG

Placebo once daily of oral tablet formulation to be taken in the morning, one hour before breakfast, with a glass of water.

Eligibility

Sex: ALLMin age: 18 YearsMax age: 65 Years

Medical Language ↔ Plain English

Inclusion Criteria A patient who met the following inclusion criteria was eligible to participate in the study: 1. Males or females with simple or complex partial seizures with or without secondary generalization, or primary generalized tonic-clonic seizures according to the International League against Epilepsy classification. Patient records were to document the frequency of seizure. 2. Age: 18 to 65 years. 3. Race: any. 4. Patients receiving up to two additional anti-epileptic medications at doses that were stable for at least the four weeks immediately preceding baseline. 5. Patients willing and able to co-operate with the study procedures including completion of patient diaries. 6. Patients living at home with a partner or carer able to monitor compliance. 7. Patients giving informed consent to participate in the study. Exclusion Criteria A patient who met the following exclusion criteria was not eligible to participate in the study: 1. Pregnant or lactating women. 2. Women of childbearing potential unless (1) surgically sterile or (2) practicing effective contraception (eg, abstinence, IUD or barrier method plus hormonal method) and having a negative serum beta-HCG result at screening and being willing to remain on the current form of contraception for the duration of the study. Postmenopausal women could be included but were to have been amenorrhoeic for at least 12 months to be considered as not being of child-bearing potential. 3. Fertile men not willing to use reliable contraception or with partners not willing to use reliable contraception. 4. Patients with status epilepticus within the past 24 months. 5. Patients with unstable abnormalities of the hepatic, renal, cardiovascular, respiratory, abdominal, haematological, endocrine or metabolic systems which might complicate assessment of the tolerability of the study medication. 6. Patients with significantly elevated liver enzymes (abnormal bilirubin level, or serum transaminase levels more than 1.5 times the upper limit of normal). 7. Patients taking drugs other than anti-epileptic agents which induce the enzyme cytochrome P450 3A4 (since these might reduce the plasma concentration of E2007), including dexamethasone, rifabutin, rifampacin, St John's Wort. 8. Patients with past or present drug or alcohol abuse. 9. Patients with unstable psychiatric illness. 10. Patients who had received an investigational drug within the three months before baseline. 11. Patients without a reliable partner or carer. 12. Patients with any condition which would make the patient, in the opinion of the investigator, unsuitable for the study.

Locations (1)

3ClinicalResearch AG

Hennigsdorf, Germany

Outcomes

Primary Outcomes

Number of participants with Treatment Emergent Adverse Events (TEAEs)

The TEAEs were defined as those Adverse Events (AEs) that start on or after the first dose of the treatment until the end of the study. AEs were classified by the investigator as 'not related', 'possibly related' or 'probably related'.

Time frame: From administration of first dose of study drug up until 42 days.

Clinical Global Impression of Tolerability (CGIT)

The investigator's global impressions of the tolerability of the study treatment was based on a five point scale: 1 - very good, 2 - good, 3 - moderate, 4 - poor, and 5 - very poor.

Time frame: Day 28

Pharmacokinetic Parameter: Area Under the Curve (AUC)(0-24hr) of E2007

Standard pharmacokinetic parameters for E2007 were derived from plasma drug concentrations in epileptic participants. A measure of systemic drug exposure over 24 hours, which is obtained by collecting a series of blood samples and measuring the concentrations of drug in each sample.

Time frame: Day 1 and Day 14

Pharmacokinetic Parameter: Cmax (Maximum Observed Plasma Concentration) of E2007

Standard pharmacokinetic parameters for E2007 were derived from plasma drug concentrations in epileptic participants. The maximum concentration of a drug observed after its administration.

Time frame: Day 1 and Day 14

Pharmacokinetic Parameter: Tmax (Time to Maximum Concentration) of E2007

Standard pharmacokinetic parameters for E2007 were derived from plasma drug concentrations in epileptic participants. The time after dosing when a drug attains its highest measurable concentration (Cmax).

Time frame: Day 1 and Day 14

Pharmacokinetic Parameter: Css,min (Minimum Steady State Plasma Concentration) of E2007

Standard pharmacokinetic parameters for E2007 were derived from plasma drug concentrations in epileptic participants. Lowest plasma concentration within a steady-state dosing interval.

Data from ClinicalTrials.gov

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Secondary Outcomes

Change from Baseline of Bond and Lader Scale

The Bond and Lader visual analogue mood scale (VAMS) had a score from 0 - 100; a higher score represented worsening of the participants condition attributed to 3 factors, (1) Anxiety (e.g., calmness), (2) Sedation (e.g., alertness, (3) Dysphoria (e.g., contentedness). The change was visit minus baseline.

Time frame: Baseline, Day 28 and Day 42

Change from Baseline of Peak Saccadic Velocity (PSV)

Saccadic velocity is the rate of eye movement in response to stimulus. The saccadic eye movement was used to allow comparison of any sedative effects seen.

Time frame: Baseline, Day 28, Day 42

Number of Particpants receiving other Anti-epileptic agents During Treatment

Time frame: Day 1 and Day 14

Percent Change from Baseline of Failed Saccades

Failed saccades is stimulus resulting in no eye movement above a defined threshold within a specified time.

Time frame: Baseline, Day 28, Day 42

Mean trough concentrations of E2007

Time frame: Day 7, Day 21, and Day 28

Number of seizures

Time frame: Baseline (Day-1) to Day 42

The Clinical Global Impression of Change

Time frame: Day 28