ZYN002 Cannabidiol Transdermal Gel in Children and Adolescents with Developmental and Epileptic Encephalopathies: An Open?label Clinical Trial [BELIEVE (ZYN2-CL-25)]
Abstract number :
Submission category :
7. Antiepileptic Drugs / 7B. Clinical Trials
Submission ID :
Presentation date :
12/7/2020 1:26:24 PM
Published date :
Nov 21, 2020, 08:24 AM
Ingrid Scheffer, The University of Melbourne and The Royal Children’s Hospital and the Florey Institute and Murdoch Children's Research Institute; Joseph Hulihan - Paradigm Neuroscience; John Messenheimer - Consultant; Shayma Ali - University of Otago; Ng
The developmental and epileptic encephalopathies (DEE) are the most severe group of epilepsies. Children have drug-resistant seizures, developmental slowing often with regression (varying from learning difficulties to mild to profound intellectual disability), and psychiatric (autism spectrum disorder, psychosis, depression, behavioral problems) and motor disabilities (cerebral palsy and movement disorders). BELIEVE (ZYN2-CL-025) evaluated the safety, tolerability, and eﬃcacy of cannabidiol (CBD) transdermal gel in children and adolescents with DEEs.
BELIEVE was an exploratory open‐label, multiple‐dose study of ZYN002 cannabidiol (CBD) transdermal gel in children and adolescents with DEEs aged 3 to < 18 years. Weight-based doses of ZYN002 125, 250, 375, or 500 mg were applied every 12 hours during a 26‐week treatment period. Following a 4-week baseline period, children were treated with ZYN002 at a twice daily dose of 125mg (< 25kg) or 250mg ( >25kg). Doses could be titrated up to a dose of 375mg (< 25kg) or 500mg ( >25kg) twice a day. Primary outcomes were safety and median percent change from baseline in the monthly (28‐day) seizure frequency over 26 weeks. Caregivers used daily diaries to record the number of countable seizures by seizure type. Absence, myoclonic, and focal aware (non‐motor) seizures were also evaluated daily. Safety and tolerability assessments included adverse events, examination of skin, vital signs, and clinical laboratory tests.
Of the 48 participants (26 male) enrolled and analyzed for safety, 46 were evaluated for eﬃcacy in the 26‐week treatment period. Median age was 10 (range 3‐16) years. Twenty-nine (60.4%) patients had at least 1 treatment-related adverse event over 26 weeks, of which 93% were mild or moderate. The most frequent were application site dryness, application site pain, and somnolence, each 8.3%. The percentage of patients with a new onset drug-related adverse event decreased from 38% at Week 4 to 3% at Week 26. In 33 patients with focal impaired awareness seizures and/or tonic-clonic seizures at baseline, there was up to 58% median monthly reduction in these seizure types from Week 8 to Week 26 and up to 63% of these patients experienced a ≥50% reduction in monthly seizure frequency during this time period.
ZYN002 CBD transdermal gel was well tolerated and data suggest reduced seizure frequency in children and adolescents with a DEE. This positive benefit‐risk profile supports further study of ZYN002 in this difficult to treat population.
:This research was funded by Zynerba Pharmaceuticals, Inc.