Antiepileptic Efficacy Study of GWP42003-P in Children and Young Adults With Dravet Syndrome (GWPCARE1)

Last updated: September 22, 2022
Sponsor: Jazz Pharmaceuticals
Overall Status: Completed

Phase

3

Condition

Epilepsy

Dravet Syndrome

Seizure Disorders (Pediatric)

Treatment

N/A

Clinical Study ID

NCT02091375
GWEP1332 Part B
2014-002941-23
  • Ages 2-18
  • All Genders

Study Summary

To investigate the potential antiepileptic effects of cannabidiol (GWP42003-P) in children and young adults with Dravet syndrome.

Eligibility Criteria

Inclusion

Key Inclusion Criteria:

  • Participants were male or female aged between 2 and 18 years (inclusive).
  • Participants had a documented history of Dravet Syndrome that was not completelycontrolled by current antiepileptic drugs.
  • Participants took one or more antiepileptic drugs at a dose that had been stable forat least four weeks.
  • All medications or interventions for epilepsy (including ketogenic diet and vagusnerve stimulation) were stable for four weeks prior to screening and participants werewilling to maintain a stable regimen throughout the study.

Exclusion

Key Exclusion Criteria:

  • Participants had clinically significant unstable medical conditions other thanepilepsy.
  • Participants had clinically relevant symptoms or a clinically significant illness inthe four weeks prior to screening or randomization, other than epilepsy.
  • Participants were currently using or had in the past used recreational or medicinalcannabis or synthetic cannabinoid based medications (including Sativex®) within thethree months prior to study entry and were unwilling to abstain for the duration forthe study.
  • Participants had any known or suspected hypersensitivity to cannabinoids or any of theexcipients of the investigational medicinal products.
  • Participants had been part of a previous clinical trial involving anotherinvestigational product in the previous six months.
  • There were plans for the participants to travel outside their country of residenceduring the study.
  • Participants previously randomized into this study. In particular, participants whoparticipated in Part A of the study could not enter Part B.

Study Design

Total Participants: 120
Study Start date:
March 30, 2015
Estimated Completion Date:
November 26, 2015

Study Description

GWEP1332 Part B recruited an entirely new group of participants than GWEP1332 Part A. Participants who failed the entry criteria for Part A were eligible to take part in Part B.

Part B was a 1:1 randomized, double-blind, placebo-controlled, 14-week comparison of GWP42003-P versus placebo. The aim of Part B was to assess the antiepileptic efficacy of GWP42003-P as an adjunctive antiepileptic treatment compared with placebo, with respect to the percentage change from baseline during the treatment period of the study in convulsive seizure frequency in children and young adults.

Following the establishment of initial eligibility and baseline measurements, participants entered Part B and began a 28-day baseline observation period.

Eligible participants were then randomized to receive either GWP42003-P or placebo on a 1:1 basis and titrated up to the target dose that was identified in Part A (up to 20 milligrams [mg] per kilogram [kg] per day), which was confirmed following completion of Part A by an independent Data Safety Monitoring Committee who reviewed unblinded safety and pharmacokinetic data from Part A.

Participants received investigational medicinal product for 14 weeks, consisting of a titration period followed by a 12-week maintenance period.

Efficacy and safety were monitored at various clinic visits and via telephone. After 14 weeks of treatment, all participants were offered the option of entering an open label extension (OLE) study. Entry was within seven days of the final treatment visit. Participants who did not immediately enter the OLE study commenced a down-titration taper period lasting up to 10 days. The taper period was interrupted if the participant wished to enter the open label extension study within the seven-day timeframe.

For participants who opted not to enter the OLE study, a follow-up telephone call was made 28 days after the end of dosing and weekly safety telephone calls were made during the 28-day follow-up period.

Connect with a study center

  • Marseille, 13385
    France

    Site Not Available

  • Paris, 75015
    France

    Site Not Available

  • Strasbourg, 67098
    France

    Site Not Available

  • Toulouse, 70034
    France

    Site Not Available

  • Gdańsk, 80-952
    Poland

    Site Not Available

  • Kraków, 30-349
    Poland

    Site Not Available

  • Glasgow, G51 4TF
    United Kingdom

    Site Not Available

  • Liverpool, L12 2AP
    United Kingdom

    Site Not Available

  • London, WC1N 3JH
    United Kingdom

    Site Not Available

  • Miami, Florida 33155
    United States

    Site Not Available

  • Orlando, Florida 32819
    United States

    Site Not Available

  • Atlanta, Georgia 30328
    United States

    Site Not Available

  • Chicago, Illinois 60611
    United States

    Site Not Available

  • Iowa City, Iowa 52242
    United States

    Site Not Available

  • Boston, Massachusetts 02114
    United States

    Site Not Available

  • Rochester, Minnesota 55905
    United States

    Site Not Available

  • NYU Comprehensive Epilepsy Center

    NY, New York 10016
    United States

    Site Not Available

  • New York, New York 10016
    United States

    Site Not Available

  • Winston-Salem, North Carolina 27408
    United States

    Site Not Available

  • Columbus, Ohio 43205
    United States

    Site Not Available

  • Philadelphia, Pennsylvania 19104
    United States

    Site Not Available

  • Houston, Texas 77030
    United States

    Site Not Available

  • Salt Lake City, Utah 84113
    United States

    Site Not Available

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