TY - JOUR
T1 - Long-term safety and efficacy of cannabidiol in children and adults with treatmentresistant Lennox-Gastaut syndrome or Dravet syndrome
T2 - Expanded access program results
AU - Laux, Linda C.
AU - Bebin, E. Martina
AU - Checketts, Daniel
AU - Chez, Michael
AU - Flamini, Robert
AU - Marsh, Eric D.
AU - Miller, Ian
AU - Nichol, Kathryn
AU - Park, Yong D
AU - Segal, Eric
AU - Seltzer, Laurie
AU - Szaflarski, Jerzy P.
AU - Thiele, Elizabeth A.
AU - Weinstock, Arie
N1 - Funding Information:
In the past two years, L.C. Laux is a Principal Investigator for GW Pharma Ltd and Zogenix. E. Martina Bebin has served on an advisory panel for GW Pharmaceuticals and is a clinical investigator on the GW1521 clinical trial. Dr. Bebin is Director of the EAP pediatric program at the University of Alabama Birmingham, which is supported by the State of Alabama. D. Checketts is an employee of GW Research Ltd. M. Chez has been a clinical investigator for the EAP study and the GWEP1332 trial, receiving support from GW Research. He has been a consultant to GW Pharmaceuticals and served as speaker for Greenwich Biosciences. R. Flamini received funding from GW Research Ltd for activities associated with his site’s individual EAP (the State of Georgia funds part of the Georgia State EAP) and is a principle investigator for GW Research studies. E.D. Marsh has been a PI on GW Pharma and Zogenix studies. Dr. Marsh has received grant funding from Zogenix Pharma, GW Pharma, National Institutes of Health, Rett Syndrome Research Trust, RettSyndrome.org, and the Commonwealth of Pennsylvania. He also has served as consultant for Stoke Therapeutics. I. Miller has received research support, travel funds, or consulting fees from: Biomarin, Dravet Syndrome Foundation, Greenwich Biosciences, Hope for HH Foundation, Insys Therapeudics, Insightec, Inc., NeuroPace, Inc., Neurelis, Inc., Tuberous Sclerosis Alliance, Ultragenyx, Upsher-Smith, and Zogenix. K Nichol is employed by Greenwich Biosciences, Inc. Y. Park served as Principal Investigator on the GWEP 1414 and 1415 clinical trials and leads the pediatric EAP program at Augusta University, which is funded by the State of Georgia. E. Segal has served as a speaker for GW Pharmaceuticals, Eisai Pharmaceuticals, Nutricia, Novartis, Lundbeck, and Lineagen. Dr. Segal has served as a consultant for GW Pharmaceuticals, Celgene, Encoded Therapeutics, qBiomed, and Epitel. He has served on Advisory Boards for GW Pharmaceuticals, Zogenix, and Aquestive. L. Seltzer is the site Principal Investigator for the EAP at the University of Rochester, supported by GW Pharmaceuticals and New York State. She is also the site Principal Investigator for GW Pharmaceuticals GW1521 and Shire Pharmaceuticals SPD489 clinical trials. J.P. Szaflarski has received funding from the National Institutes of Health, the National Science Foundation, Shor Foundation for Epilepsy Research, EFA, U.S. Department of Defense, UCB Biosciences, NeuroPace Inc., SAGE Therapeutics Inc., Greenwich Biosciences Inc., Serina Therapeutics Inc., and Eisai, Inc. Dr. Szaflarski has served as a consultant for SAGE Therapeutics Inc., Greenwich Biosciences Inc., NeuroPace, Inc., Upsher-Smith Laboratories, Inc., Medical Association of the State of Alabama, Serina Therapeutics Inc., LivaNova Inc., Lundbeck, and Elite Medical Experts LLC. He currently serves as an editorial board member for Epilepsy & Behavior, Journal of Epileptology (Associate Editor), Restorative Neurology and Neuroscience (Associate Editor), Journal of Medical Science, Epilepsy Currents (Contributing Editor), and Folia Medica Copernicana. E.A. Thiele serves as consultant to GW Pharmaceuticals companies, Aquestive, Ovid, Upsher Smith, West Therapeutics, and Zogenix. She has served as an investigator in the DS, LGS and TSC clinical trials, and received funding from GW Pharma for the expanded access program. A. Weinstock is the Director of the EAP program at the University at Buffalo, NY, which is supported by the New York State Department of Health and serves as a paid speaker for Greenwich Biosciences Inc. We confirm that we have read the Journal’s position on issues involved in ethical publication and affirm that this report is consistent with those guidelines.
Publisher Copyright:
© 2019
PY - 2019/8
Y1 - 2019/8
N2 - Background: Since 2014, patients with severe treatment-resistant epilepsies (TREs) have been receiving add-on cannabidiol (CBD) in an ongoing, expanded access program (EAP), which closely reflects clinical practice. We conducted an interim analysis of long-term efficacy and tolerability in patients with Lennox-Gastaut syndrome (LGS) or Dravet syndrome (DS) who received CBD treatment through December 2016. Methods: Children and adults with LGS/DS taking stable doses of antiepileptic drugs (AEDs) at baseline were included from 25 EAP sites across the United States. During the 4-week baseline period, parents/caregivers kept diaries of all countable seizure types. Patients received a pharmaceutical formulation of highly purified CBD (Epidiolex®; 100 mg/mL) in oral solution at 2–10 mg/kg/day, titrated until tolerability limit or a maximum dose of 25–50 mg/kg/day. Patient visits were every 2–4 weeks. The percentage change from baseline in median monthly convulsive (ie, major motor) and total seizures was evaluated at 12-week intervals through 96 weeks. The percentages of patients who had ≥50%, ≥75%, and 100% reduction in monthly seizures relative to the baseline period were also evaluated. Adverse events (AEs) were monitored and summarized for the safety analysis set (SAS) through 144 weeks. Results: Of the 607 patients in the SAS, 58 had DS and 94 had LGS (N = 152); 455 patients had other TREs. Twenty-eight percent of LGS/DS patients withdrew, primarily owing to lack of efficacy (20%). LGS/DS patients were taking a median of 3 (0–10) concomitant AEDs. Median treatment duration was 78.3 (range, 4.1–146.4) weeks. Between weeks 12 and 96, median CBD dose ranged from 21 to 25 mg/kg/day. At 12 weeks, add-on CBD reduced median monthly major motor seizures by 50% and total seizures by 44%, with consistent reductions in both seizure types through 96 weeks. At 12 weeks, the proportions of patients with ≥50%, ≥75%, and 100% reductions in major motor seizures were 53%, 23%, and 6%; the proportions with corresponding reductions in total seizures were 46%, 26%, and 5%. Responder rates for both seizure types were consistent through 96 weeks. CBD had an acceptable safety profile; the most common AEs were somnolence (30%) and diarrhea (24%). Conclusions: Results from this interim analysis support add-on CBD as an effective long-term treatment option in LGS or DS.
AB - Background: Since 2014, patients with severe treatment-resistant epilepsies (TREs) have been receiving add-on cannabidiol (CBD) in an ongoing, expanded access program (EAP), which closely reflects clinical practice. We conducted an interim analysis of long-term efficacy and tolerability in patients with Lennox-Gastaut syndrome (LGS) or Dravet syndrome (DS) who received CBD treatment through December 2016. Methods: Children and adults with LGS/DS taking stable doses of antiepileptic drugs (AEDs) at baseline were included from 25 EAP sites across the United States. During the 4-week baseline period, parents/caregivers kept diaries of all countable seizure types. Patients received a pharmaceutical formulation of highly purified CBD (Epidiolex®; 100 mg/mL) in oral solution at 2–10 mg/kg/day, titrated until tolerability limit or a maximum dose of 25–50 mg/kg/day. Patient visits were every 2–4 weeks. The percentage change from baseline in median monthly convulsive (ie, major motor) and total seizures was evaluated at 12-week intervals through 96 weeks. The percentages of patients who had ≥50%, ≥75%, and 100% reduction in monthly seizures relative to the baseline period were also evaluated. Adverse events (AEs) were monitored and summarized for the safety analysis set (SAS) through 144 weeks. Results: Of the 607 patients in the SAS, 58 had DS and 94 had LGS (N = 152); 455 patients had other TREs. Twenty-eight percent of LGS/DS patients withdrew, primarily owing to lack of efficacy (20%). LGS/DS patients were taking a median of 3 (0–10) concomitant AEDs. Median treatment duration was 78.3 (range, 4.1–146.4) weeks. Between weeks 12 and 96, median CBD dose ranged from 21 to 25 mg/kg/day. At 12 weeks, add-on CBD reduced median monthly major motor seizures by 50% and total seizures by 44%, with consistent reductions in both seizure types through 96 weeks. At 12 weeks, the proportions of patients with ≥50%, ≥75%, and 100% reductions in major motor seizures were 53%, 23%, and 6%; the proportions with corresponding reductions in total seizures were 46%, 26%, and 5%. Responder rates for both seizure types were consistent through 96 weeks. CBD had an acceptable safety profile; the most common AEs were somnolence (30%) and diarrhea (24%). Conclusions: Results from this interim analysis support add-on CBD as an effective long-term treatment option in LGS or DS.
KW - Cannabidiol
KW - Dravet syndrome
KW - Efficacy
KW - Expanded access program
KW - Lennox-Gastaut syndrome
KW - Seizures
KW - Tolerability
KW - Treatment-resistant epilepsy
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U2 - 10.1016/j.eplepsyres.2019.03.015
DO - 10.1016/j.eplepsyres.2019.03.015
M3 - Article
C2 - 31022635
AN - SCOPUS:85064518196
SN - 0920-1211
VL - 154
SP - 13
EP - 20
JO - Journal of Epilepsy
JF - Journal of Epilepsy
ER -
