1. A multicenter Phase II randomized, placebo-controlled single-blind trial with the SV2A ligand seletracetam in photosensitive epilepsy patients.
- Author
-
Kasteleijn-Nolst Trenité D, Stockis A, Hirsch E, Genton P, Abou-Khalil BW, French JA, Masnou P, and Löscher W
- Abstract
The objective of this study was to evaluate the effect of seletracetam (SEL), a potent modulator of synaptic vesicle glycoprotein 2A (SV2A), in patients with photoparoxysmal EEG response (PPR) to intermittent photic stimulation (IPS) as proof-of-principle of efficacy in patients with epilepsy. In this multicenter, single-blind Phase II study, adults with photosensitive epilepsy, with/without concomitant antiseizure medication therapy, underwent IPS under 3 eye conditions (at eye closure, eyes closed and eyes open) after a single oral dose of placebo (day - 1) or SEL (day 1; 0.5, 1, 2, 4, 10, or 20 mg). Complete suppression was a standardized photosensitivity range reduction to 0 over ≥ 1 time points for all eye conditions. Partial suppression was a ≥ 3-point reduction over ≥ 3 testing times vs the same time points on day - 1 in ≥ 1 eye condition. In addition, pharmacokinetics and safety were assessed. Of 27 evaluable patients, 9 reentered to receive a 2nd dosing 1-6 months later, providing a total of 36 individual exposures. At all doses administered - even the lowest -, several subjects reached a complete abolishment of PPR, with a rapid onset of effect. Overall, complete abolishment of PPR was obtained in 40-71 % of the patients; the effect increasing with the dose. In terms of effective doses to suppress PPR, SEL was at least 1,500 times more potent than levetiracetam and 10-20 times more potent than brivaracetam. Adverse events of SEL, including dizziness and somnolence, were mild to moderate. Pharmacokinetics of SEL demonstrated rapid absorption and a linear dose:plasma level relationship. This proof-of-principle study demonstrates that - based on our own experience - SEL is the most potent compound ever tested in the photosensitivity model., Competing Interests: Declaration of competing interest The authors declare the following financial interests/personal relationships which may be considered as potential competing interests: [D. Kasteleijn-Nolst Trenité has received in the past 5 years consultancy fees from UCB, Otsuka, SK, Jazz, and Praxis. Armel Stockis is a former employee of UCB Pharma and has received in the past 5 years consultancy fees from UCB, Roche, and EyeD Pharma. E. Hirsch has received consultancy fees from UCB, Angelini, and Jazz. Pierre Genton has received speaker invitations and honoraria from Sanofi-Aventis, Novartis, UCB, and Eisai and received support for teaching programs from Sanofi-Aventis and UCB. The institution of Dr. Abou-Khalil has received research support from Cerevel Therapeutics, Neuroelectrics, Otsuka America Pharmaceutical, SK-Pharma, UCB SA, and Xenon. J. French receives salary support from the Epilepsy Foundation and from Epilepsy Study Consortium for consulting work and/or attending Scientific Advisory Boards for Acadia Pharmaceuticals, Access Industries, Acuta Capital Partners, AFASCI Inc, Agrithera, Inc., Alterity Therapeutics Limited, Angelini Pharma S.p.A, Autifony Therapeutics Limited, Axonis Therapeutics, Baergic Bio, Beacon Biosignals, Inc., Biogen, Biohaven Pharmaceuticals, Bloom Science Inc., Bright Minds Biosciences, Inc., Camp4 Therapeutics Corporation, Capsida Biotherapeutics, Cerebral Therapeutics, Cerecin Inc., Cerevel, Ceribell, Cognizance Biomarkers, Cowen and Company, LLC, Crossject, EcoR1 Capital, Eisai, Encoded Therapeutics, Engrail, Epalex, EpiMinder, Epitel Inc, Equilibre BioPharmaceuticals, Genentech, Inc., Grin Therapeutics, Harmony/Epygenix, iQure Pharma Inc, IQVIA RDS Inc, Janssen Pharmaceutica, Jazz Pharmaceuticals, Korro Bio Inc., Leal Therapeutics Inc, Lipocine, LivaNova, Longboard Pharmaceuticals, Marinus, Modulight.bio, Neumirna Therapeutics, Neurelis, Neurocrine, NeuroPace, Inc., NeuroPro Therapeutics, Neuroventis, Neurona Therapeutics, Neurvati, Noema, Ono Pharmaceutical Co., Otsuka Pharmaceutical Development, Ovid Therapeutics Inc., Praxis, PureTech LTY Inc., Rapport Therapeutics, Inc., Receptor Holdings Inc., Rivervest Venture Partners, Sage Therapeutics, Inc., SK Life Sciences, Stoke, Supernus, Takeda, Taysha Gene Therapies, Third Rock Ventures LLC, UCB Inc., uniQure, Ventus Therapeutics, Vida Ventures Management, Xenon. J. French has also received research support from the Epilepsy Study Consortium (Funded by Eisai and UCB,) Epilepsy Study Consortium/Epilepsy Foundation (Funded by UCB), GW/FACES/One8Foundation and NINDS. She is on the editorial board of Lancet Neurology and Neurology Today. She is Chief Medical/Innovation Officer for the Epilepsy Foundation. She is the President and on the Board of Directors for the Epilepsy Study Consortium, Inc. Pascal Masnou has nothing to disclose. W. Löscher is cofounder and CSO of PrevEp, Inc. (Bethesda, MD, USA), which currently develops an intranasal formulation of SEL (patent submitted). He has received in the past 5 years consultancy fees from Lundbeck, Angelini, Clexio, Selene, Axonis, SynapCell, Sintetica, ND Capital, Atlas Venture, Cogent Biosolutions, Ovid, Idorsia, and Addex]., (Copyright © 2024 The Authors. Published by Elsevier Inc. All rights reserved.)
- Published
- 2025
- Full Text
- View/download PDF