Your search keyword '"White, H. A."' showing total 23 results

1. Progress report on new medications for seizures and epilepsy: A summary of the 17th Eilat Conference on New Antiepileptic Drugs and Devices (EILAT XVII). II. Drugs in more advanced clinical development.

Author

Bialer, Meir, Johannessen, Svein I., Koepp, Matthias J., Perucca, Emilio, Perucca, Piero, Tomson, Torbjörn, and White, H. Steve

Subjects

INVESTIGATIONAL therapies, MENTAL depression, POTASSIUM channels, SEIZURES (Medicine), INVESTIGATIONAL drugs, EPILEPSY

Abstract

The 17th Eilat Conference on New Antiepileptic Drugs and Devices took place in Madrid, Spain on May 5–8, 2024. As usual, the core part of the conference consisted of presentations on investigational drugs at various stages of development for epilepsy‐related indications. Summaries of information on compounds in preclinical or early clinical development are included in an accompanying publication (Part I). In this article, we provide summaries for five compounds in more advanced clinical development, i.e. compounds for which some information on antiseizure activity in individuals with epilepsy is available. These investigational treatments include azetukalner (XEN1101), a potent, KV7.2/7.3‐specific potassium channel opener in development for the treatment of focal seizures, generalized tonic–clonic seizures, and major depressive disorder; bexicaserin (LP352), a selective 5‐HT2C receptor superagonist in development for the treatment of seizures associated with developmental and epileptic encephalopathies; radiprodil, a selective negative allosteric modulator of NR2B subunit‐containing N‐methyl‐D‐aspartate glutamate receptors, in development for the treatment of seizures and behavior manifestations associated with disorders caused by gain‐of‐function mutations in the GRIN1, −2A, ‐2B, or ‐2D genes; soticlestat (TAK‐935), a selective inhibitor of cholesterol 24‐hydroxylase in development for the treatment of seizures associated with Dravet syndrome and Lennox–Gastaut syndrome; and STK‐001, an antisense oligonucleotide designed to upregulate Nav1.1 protein expression and improve outcomes in individuals with Dravet syndrome. The diversity in mechanisms of action of these agents illustrates different approaches being pursued in the discovery of novel treatments for seizures and epilepsy. For two of the compounds discussed in this report (azetukalner and soticlestat), clinical evidence of efficacy has already been obtained in a randomized placebo‐controlled adjunctive‐therapy trial. For the other compounds, adequately powered placebo‐controlled efficacy trials have not been completed to date. [ABSTRACT FROM AUTHOR]

Published

2024

2. Progress report on new medications for seizures and epilepsy: A summary of the 17th Eilat Conference on New Antiepileptic Drugs and Devices (EILAT XVII). I. Drugs in preclinical and early clinical development.

Author

Bialer, Meir, Johannessen, Svein I., Koepp, Matthias J., Perucca, Emilio, Perucca, Piero, Tomson, Torbjörn, and White, H. Steve

Subjects

MEDICAL personnel, HIPPOCAMPAL sclerosis, TUBEROUS sclerosis, SODIUM channels, PARTIAL epilepsy, ANTICONVULSANTS, EPILEPSY, ANTI-NMDA receptor encephalitis, HYDROXYCINNAMIC acids

Abstract

For >30 years, the Eilat Conference on New Antiepileptic Drugs and Devices has provided a forum for the discussion of advances in the development of new therapies for seizures and epilepsy. The EILAT XVII conference took place in Madrid, Spain, on May 5–8, 2024. Participants included basic scientists and clinical investigators from industry and academia, other health care professionals, and representatives from lay organizations. We summarize in this article information on treatments in preclinical and in early clinical development discussed at the conference. These include AMT‐260, a gene therapy designed to downregulate the expression of Glu2K subunits of kainate receptors, in development for the treatment of drug‐resistant seizures associated with mesial temporal sclerosis; BHV‐7000, a selective activator of heteromeric Kv7.2/7.3 potassium channels, in development for the treatment of focal epilepsy; ETX101, a recombinant adeno‐associated virus serotype 9 designed to increase NaV1.1 channel density in inhibitory γ‐aminobutyric acidergic (GABAergic) neurons, in development for the treatment of SCN1A‐positive Dravet syndrome; GAO‐3‐02, a compound structurally related to synaptamide, which exerts antiseizure activity at least in part through an action on cannabinoid type 2 receptors; LRP‐661, a structural analogue of cannabidiol, in development for the treatment of seizures associated with Lennox–Gastaut syndrome, Dravet syndrome, and tuberous sclerosis complex; OV329, a selective inactivator of GABA aminotransferase, in development for the treatment of drug‐resistant seizures; PRAX‐628, a functionally selective potent sodium channel modulator with preference for the hyperexcitable state of sodium channels, in development for the treatment of focal seizures; RAP‐219, a selective negative allosteric modulator of transmembrane α‐amino‐3‐hydroxy‐5‐methyl‐4‐isoxazolepropionic acid receptor regulatory protein γ‐8, in development for the treatment of focal seizures; and rozanolixizumab, a humanized anti‐neonatal Fc receptor monoclonal antibody, in development for the treatment of LGI1 autoimmune encephalitis. Treatments in more advanced development are summarized in Part II of this report. [ABSTRACT FROM AUTHOR]

Published

2024

3. Brief history of anti‐seizure drug development

Author

Rho, Jong M and White, H Steve

Subjects

Biomedical and Clinical Sciences, Neurosciences, Clinical Sciences, Epilepsy, Clinical Research, Brain Disorders, Health Services, Neurodegenerative, Development of treatments and therapeutic interventions, 5.1 Pharmaceuticals, Neurological, Anti‐convulsant, Anti‐epileptic drug, Anti‐seizure drug, Drug development, History, Medication, Clinical sciences, Biological psychology

Abstract

The mainstay of therapy for epilepsy is anti-seizure drugs (ASDs, also referred to as anticonvulsants and anti-epileptic medications). Through much of the past century, only a handful for ASDs were available for clinical use. However, with the creation of the U.S. National Institutes of Health/National Institute of Neurological Disorders and Stroke (NINDS)-sponsored Anticonvulsant Screening Program (ASP), coupled with the emergence of high-throughput screening platforms and methodologies, and advances in our understanding of the fundamental neurobiology of epilepsy, ASD development has greatly accelerated over the past 25 years. More than 18 new ASDs have been approved for clinical use since the inception of the ASP. Despite this remarkable success and the emergence of drugs possessing more favorable pharmacokinetic profiles that act on novel molecular targets, there has been increasing recognition that the paradigms for drug discovery have not yielded significant improvements in therapeutic efficacy, and that disease modification (i.e., anti-epileptogenesis), among other challenges, must be addressed. Thus, with the renewed framework and mission of improving the lives of people with epilepsy, the name of the ASP was changed to the Epilepsy Therapy Screening Program (ETSP). This review briefly summarizes the history of ASD development and outlines some of the challenges and opportunities for the next generation of drug therapies for the epilepsy field.

Published

2018

4. Progress report on new antiepileptic drugs: A summary of the Sixteenth Eilat Conference on New Antiepileptic Drugs and Devices (EILAT XVI): II. Drugs in more advanced clinical development.

Author

Bialer, Meir, Johannessen, Svein I., Koepp, Matthias J., Levy, René H., Perucca, Emilio, Perucca, Piero, Tomson, Torbjörn, and White, H. Steve

Subjects

ANTICONVULSANTS, GOVERNMENT agencies, DRUGS, BUMETANIDE, TEMPORAL lobectomy, CONFERENCES & conventions

Abstract

The Sixteenth Eilat Conference on New Antiepileptic Drugs and Devices (EILAT XVI) was held in Madrid, Spain on May 22–25, 2022 and was attended by 157 delegates from 26 countries representing basic and clinical science, regulatory agencies, and pharmaceutical industries. One day of the conference was dedicated to sessions presenting and discussing investigational compounds under development for the treatment of seizures and epilepsy. The current progress report summarizes recent findings and current knowledge for seven of these compounds in more advanced clinical development for which either novel preclinical or patient data are available. These compounds include bumetanide and its derivatives, darigabat, ganaxolone, lorcaserin, soticlestat, STK‐001, and XEN1101. Of these, ganaxolone was approved by the US Food and Drug Administration in March 2022 for the treatment of seizures associated with cyclin‐dependent kinase‐like 5 deficiency disorder in patients 2 years of age and older. [ABSTRACT FROM AUTHOR]

Published

2022

5. Progress report on new antiepileptic drugs: A summary of the Sixteenth Eilat Conference on New Antiepileptic Drugs and Devices (EILAT XVI): I. Drugs in preclinical and early clinical development.

Author

Bialer, Meir, Johannessen, Svein I., Koepp, Matthias J., Levy, René H., Perucca, Emilio, Perucca, Piero, Tomson, Torbjörn, and White, H. Steve

Subjects

ANTICONVULSANTS, EPILEPSY, DRUG target, DRUG therapy, GOVERNMENT agencies, DRUGS

Abstract

The Eilat Conferences have provided a forum for discussion of novel treatments of epilepsy among basic and clinical scientists, clinicians, and representatives from regulatory agencies as well as from the pharmaceutical industry for 3 decades. Initially with a focus on pharmacological treatments, the Eilat Conferences now also include sessions dedicated to devices for treatment and monitoring. The Sixteenth Eilat Conference on New Antiepileptic Drugs and Devices (EILAT XVI) was held in Madrid, Spain, on May 22–25, 2022 and was attended by 157 delegates from 26 countries. As in previous Eilat Conferences, the core of EILAT XVI consisted of a sequence of sessions where compounds under development were presented and discussed. This progress report summarizes preclinical and, when available, phase 1 clinical data on five different investigational compounds in preclinical or early clinical development, namely GAO‐3‐02, GRT‐X, NBI‐921352 (formerly XEN901), OV329, and XEN496 (a pediatric granular formulation of retigabine/ezogabine). Overall, the data presented in this report illustrate novel strategies for developing antiseizure medications, including an interest in novel molecular targets, and a trend to pursue potential new treatments for rare and previously neglected severe epilepsy syndromes. [ABSTRACT FROM AUTHOR]

Published

2022

6. Development of an antiepileptogenesis drug screening platform: Effects of everolimus and phenobarbital.

Author

Barker‐Haliski, Melissa, Knox, Kevin, Zierath, Dannielle, Koneval, Zachery, Metcalf, Cameron, Wilcox, Karen S., and White, H. Steve

Subjects

PHENOBARBITAL, DRUG development, ANIMAL disease models, SPRAGUE Dawley rats

Abstract

Objective: The kainic acid (KA)‐induced status epilepticus (SE) model in rats is a well‐defined model of epileptogenesis. This model closely recapitulates many of the clinical and pathological characteristics of human temporal lobe epilepsy (TLE) that arise following SE or another neurological insult. Spontaneous recurrent seizures (SRS) in TLE can present after a latent period following a neurological insult (traumatic brain injury, SE event, viral infection, etc.). Moreover, this model is suitable for preclinical studies to evaluate the long‐term process of epileptogenesis and screen putative disease‐modifying/antiepileptogenic agents. The burden of human TLE is highly variable, similar to the post‐KA SE rat model. In this regard, this model may have broad translational relevance. This report thus details the pharmacological characterization and methodological refinement of a moderate‐throughput drug screening program using the post‐KA‐induced SE model of epileptogenesis in male Sprague Dawley rats to identify potential agents that may prevent or modify the burden of SRS. Specifically, we sought to demonstrate whether our protocol could prevent the development of SRS or lead to a reduced frequency/severity of SRS. Methods: Rats were administered either everolimus (2–3 mg/kg po) beginning 1, 2, or 24 h after SE onset, or phenobarbital (60 mg/kg ip) beginning 1 h after SE onset. All treatments were administered once/day for 5–7 days. Rats in all studies (n = 12/treatment dose/study) were then monitored intermittently by video‐electroencephalography (2 weeks on, 2 weeks off, 2 weeks on epochs) to determine latency to onset of SRS and disease burden. Results: Although no adverse side effects were observed in our studies, no treatment significantly modified disease or prevented the presentation of SRS by 6 weeks after SE onset. Significance: Neither phenobarbital nor everolimus administered at several time points after SE onset prevented the development of SRS. Nonetheless, we demonstrate a practical and moderate‐throughput screen for potential antiepileptogenic agents in a rat model of TLE. [ABSTRACT FROM AUTHOR]

Published

2021

7. Progress report on new antiepileptic drugs: A summary of the Fifteenth Eilat Conference on New Antiepileptic Drugs and Devices (EILAT XV). II. Drugs in more advanced clinical development.

Author

Bialer, Meir, Johannessen, Svein I., Koepp, Matthias J., Levy, René H., Perucca, Emilio, Perucca, Piero, Tomson, Torbjörn, and White, H. Steve

Subjects

ANTICONVULSANTS, FENFLURAMINE, DRUGS, SEIZURES (Medicine), PROGRESS

Abstract

The Fifteenth Eilat Conference on New Antiepileptic Drugs and Devices (EILAT XV) was held as a fully virtual conference from July 27 to July 30, 2020 for the sessions on drugs, and on August 3, 2020 for the sessions on devices. A total of 534 delegates from 63 countries attended lectures and interactive discussions, representing a broad range of disciplines from basic science, clinical research, and clinical care. This progress report provides summaries of recent findings on investigational compounds for which preclinical data as well as data from patient studies were presented. The report includes the following five compounds: anakinra, cenobamate, CVL‐865, fenfluramine, and ganaxolone, all with novel modes of action compared to more established antiepileptic drugs. Some of these compounds demonstrated promising results in placebo‐controlled phase 3 trials, and two have recently received approval from the US Food and Drug Administration (FDA). These include cenobamate, which was approved by the FDA on November 21, 2019 for the treatment of partial onset (focal) seizures in adults, and fenfluramine oral solution, which was approved by the FDA on June 25, 2020 for the treatment of seizures associated with Dravet syndrome in patients 2 years and older. [ABSTRACT FROM AUTHOR]

Published

2020

8. Progress report on new antiepileptic drugs: A summary of the Fourteenth Eilat Conference on New Antiepileptic Drugs and Devices (EILAT XIV). I. Drugs in preclinical and early clinical development.

Author

Bialer, Meir, Johannessen, Svein I., Koepp, Matthias J., Levy, René H., Perucca, Emilio, Tomson, Torbjörn, and White, H. Steve

Subjects

ANTICONVULSANTS, ADENOSINES, ADENOSINE kinase, DRUG development, KETONES

Abstract

Summary: The Fourteenth Eilat Conference on New Antiepileptic Drugs and Devices (EILAT XIV) took place in Madrid, Spain, on May 13‐16, 2018 and was attended by 168 delegates from 28 countries. The conference provided a forum for professionals involved in basic science, clinical research, regulatory affairs, and clinical care to meet and discuss the latest advances related to discovery and development of drugs and devices aimed at improving the management of people with epilepsy. This progress report provides a summary of findings on investigational compounds for which data from preclinical or early (phase I) clinical studies were presented. The compounds reviewed include adenosine and adenosine kinase inhibitors, BIS‐001 (huperzine A), 2‐deoxy‐d‐glucose, FV‐082, FV‐137, JNJ‐40411813, JNJ‐55511118 and analogs, ketone‐enhanced antiepileptic drugs, oxynytones, OV329, TAK‐935 (OV935), XEN901, and XEN1101. Many innovative approaches to drug development were presented. For example, some compounds are being combined with traditional antiepileptic drugs based on evidence of synergism in seizure models, some act as inhibitors of enzymes involved in modulation of neuronal activity, and some interact in novel ways with excitatory receptors or ion channels. Some of the compounds in development target the etiology of specific epilepsy syndromes (including orphan conditions) through precision medicine, and some offer hope of producing disease‐modifying effects rather than symptomatic seizure suppression. Overall, the results summarized in the report indicate that important advances are being made in the effort to develop compounds with potentially improved efficacy and safety profiles compared with existing agents. [ABSTRACT FROM AUTHOR]

Published

2018

9. Progress report on new antiepileptic drugs: A summary of the Fourteenth Eilat Conference on New Antiepileptic Drugs and Devices (EILAT XIV). II. Drugs in more advanced clinical development.

Author

Bialer, Meir, Johannessen, Svein I., Koepp, Matthias J., Levy, René H., Perucca, Emilio, Tomson, Torbjörn, and White, H. Steve

Subjects

EPILEPSY, ANTICONVULSANTS, LENNOX-Gastaut syndrome, DRUG development, PLACEBOS

Abstract

Summary: The Fourteenth Eilat Conference on New Antiepileptic Drugs and Devices (EILAT XIV) took place in Madrid, Spain, on May 13‐16, 2018 and was attended by 168 delegates from 28 countries. The conference provided a forum for professionals involved in basic science, clinical research, regulatory affairs, and clinical care to meet and discuss the latest advances related to discovery and development of drugs and devices aimed at improving the management of people with epilepsy. This progress report provides a summary of findings on investigational compounds for which data from both preclinical studies and studies in patients were presented. The compounds reviewed include anakinra, cannabidiol, cannabidivarin, fenfluramine, ganaxolone, medium‐chain fatty acids, padsevonil, and the valproic derivatives valnoctamide and sec‐butylpropylacetamide. On June 25, 2018, the US Food and Drug Administration approved a standardized formulation of cannabidiol oral solution for the treatment of seizures associated with Lennox‐Gastaut syndrome and Dravet syndrome in patients 2 years and older. The report shows that there continues to be a steady flow of potential antiepileptic drugs progressing to clinical development. Many of these compounds show innovative mechanisms of action, and some have already been tested in placebo‐controlled randomized controlled trials, with promising efficacy and safety results. [ABSTRACT FROM AUTHOR]

Published

2018

10. Progress report on new antiepileptic drugs: A summary of the Thirteenth Eilat Conference on New Antiepileptic Drugs and Devices ( EILAT XIII).

Author

Bialer, Meir, Johannessen, Svein I., Levy, René H., Perucca, Emilio, Tomson, Torbjörn, and White, H. Steve

Subjects

ANTICONVULSANTS, DRUG development, TREATMENT of epilepsy, ADENOSINES, CONFERENCES & conventions

Abstract

The Thirteenth Eilat Conference on New Antiepileptic Drugs and Devices (EILAT XIII) took place in Madrid, Spain, on June 26-29, 2016, and was attended by >200 delegates from 31 countries. The present Progress Report provides an update on experimental and clinical results for drugs presented at the Conference. Compounds for which summary data are presented include an AED approved in 2016 (brivaracetam), 12 drugs in phase I- III clinical development (adenosine, allopregnanolone, bumetanide, cannabidiol, cannabidivarin, 2-deoxy- d-glucose, everolimus, fenfluramine, huperzine A, minocycline, SAGE-217, and valnoctamide) and 6 compounds or classes of compounds for which only preclinical data are available (bumetanide derivatives, sec-butylpropylacetamide, FV-082, 1 OP-2198, NAX 810-2, and SAGE-689). Overall, the results presented at the Conference show that considerable efforts are ongoing into discovery and development of AEDs with potentially improved therapeutic profiles compared with existing agents. Many of the drugs discussed in this report show innovative mechanisms of action and many have shown promising results in patients with pharmacoresistant epilepsies, including previously neglected rare and severe epilepsy syndromes. [ABSTRACT FROM AUTHOR]

Published

2017

11. Acute cognitive impact of antiseizure drugs in naive rodents and corneal-kindled mice.

Author

Barker‐Haliski, Melissa L., Vanegas, Fabiola, Mau, Matthew J., Underwood, Tristan K., and White, H. Steve

Subjects

EPILEPSY, DRUG development, COGNITION, LABORATORY rodents, LABORATORY mice

Abstract

Objective Some antiseizure drugs ( ASDs) are associated with cognitive liability in patients with epilepsy, thus ASDs without this risk would be preferred. Little comparative pharmacology exists with ASDs in preclinical models of cognition. Few pharmacologic studies exist on the acute effects in rodents with chronic seizures. Predicting risk for cognitive impact with preclinical models may supply valuable ASD differentiation data. Methods ASDs (phenytoin [ PHT]; carbamazepine [ CBZ]; valproic acid [ VPA]; lamotrigine [ LTG]; phenobarbital [ PB]; tiagabine [ TGB]; retigabine [ RTG]; topiramate [ TPM]; and levetiracetam [ LEV]) were administered equivalent to maximal electroshock median effective dose ([ ED50]; mice, rats), or median dose necessary to elicit minimal motor impairment (median toxic dose [ TD50]; rats). Cognition models with naive adult rodents were novel object/place recognition ( NOPR) task with CF-1 mice, and Morris water maze ( MWM) with Sprague-Dawley rats. Selected ASDs were also administered to rats prior to testing in an open field. The effect of chronic seizures and ASD administration on cognitive performance in NOPR was also determined with corneal-kindled mice. Mice that did not achieve kindling criterion (partially kindled) were included to examine the effect of electrical stimulation on cognitive performance. Sham-kindled and age-matched mice were also tested. Results No ASD ( ED50) affected latency to locate the MWM platform; TD50 of PB, RTG, TPM, and VPA reduced this latency. In naive mice, CBZ and VPA ( ED50) reduced time with the novel object. Of interest, no ASD ( ED50) affected performance of fully kindled mice in NOPR, whereas CBZ and LEV improved cognitive performance of partially kindled mice. Significance Standardized approaches to the preclinical evaluation of an ASD's potential cognitive impact are needed to inform drug development. This study demonstrated acute, dose- and model-dependent effects of therapeutically relevant doses of ASDs on cognitive performance of naive mice and rats, and corneal-kindled mice. This study highlights the challenge of predicting clinical adverse effects with preclinical models. [ABSTRACT FROM AUTHOR]

Published

2016

12. Disease Modification in Epilepsy: From Animal Models to Clinical Applications.

Author

Barker-Haliski, Melissa, Friedman, Dan, French, Jacqueline, and White, H.

Subjects

THERAPEUTIC use of biochemical markers, BIOLOGICAL models, DATABASES, EPILEPSY, SYSTEMATIC reviews, DRUG development

Abstract

Several relevant animal models of epileptogenesis and biomarkers have emerged for evaluating the antiepileptogenic potential of an investigational drug. Although several promising candidate compounds and approaches have been identified in these preclinical models, no treatment has yet successfully navigated the path from preclinical efficacy to clinical validation. Until such an agent can move from preclinical proof of concept to clinical success, the need remains to continually develop and optimize preclinical models and clinical trial design in an effort to guide potential clinical investigations. This review describes several available models of disease modification and/or epileptogenesis, preclinical studies in these models and potential biomarkers useful for evaluating the efficacy of a potential therapeutic agent in the preclinical setting. The results that emerge from such efforts may then guide the clinical evaluation of a candidate compound. This review discusses some of the known limitations and hurdles to moving compounds found effective in these models to clinical practice, in the hope that knowledge of this information will facilitate the design and conduct of clinical studies and effectively facilitate the identification of a first-in-class disease-modifying or antiepileptogenic agent. [ABSTRACT FROM AUTHOR]

Published

2015

13. Development of new treatment approaches for epilepsy: Unmet needs and opportunities.

Author

French, Jacqueline A., White, H. Steve, Klitgaard, Henrik, Holmes, Gregory L., Privitera, Michael D., Cole, Andrew J., Quay, Ellinor, Wiebe, Samuel, Schmidt, Dieter, Porter, Roger J., Arzimanoglou, Alexis, Trinka, Eugen, and Perucca, Emilio

Subjects

*ANTICONVULSANTS, *TREATMENT of epilepsy, *DRUG development, *DRUG side effects, *NEUROPHARMACOLOGY

Abstract

A working group was created to address clinical 'gaps to care' as well as opportunities for development of new treatment approaches for epilepsy. The working group primarily comprised clinicians, trialists, and pharmacologists. The group identified a need for better animal models for both efficacy and tolerability, and noted that animal models for potential disease-modifying or antiepileptogenic effect should mirror conditions in human trials. For antiseizure drugs ( ASDs), current animal models have not been validated with respect to their relationship to efficacy in common epilepsy syndromes. The group performed an 'expert opinion' survey of perceived efficacy of the available ASDs, and identified a specific unmet need for ASDs to treat tonic-atonic and myoclonic seizures. No correlation has as yet been demonstrated between animal models of tolerability and adverse effects ( AEs), versus tolerability in humans. There is a clear opportunity for improved therapies in relation to dose-related AEs. The group identified common and rare epilepsy syndromes that could represent opportunities for clinical trials. They identified opportunities for antiepileptogenic ( AEG) therapies in both adults and children, acknowledging that the presence of a biomarker would substantially improve the chances of a successful trial. However, the group acknowledged that disease-modifying therapies (given after the first seizure or after the development of epilepsy) would be easier to study than AEG therapies. [ABSTRACT FROM AUTHOR]

Published

2013

14. Issues related to development of new antiseizure treatments.

Author

Wilcox, Karen S., Dixon‐Salazar, Tracy, Sills, Graeme J., Ben‐Menachem, Elinor, Steve White, H., Porter, Roger J., Dichter, Marc A., Moshé, Solomon L., Noebels, Jeffrey L., Privitera, Michael D., and Rogawski, Michael A.

Subjects

ANTICONVULSANTS, TREATMENT of epilepsy, DRUG development, NEUROPHARMACOLOGY

Abstract

This report represents a summary of the discussions led by the antiseizure treatment working group of the International League Against Epilepsy ( ILAE)/American Epilepsy Society ( AES) Working Groups joint meeting in London (London Meeting). We review here what is currently known about the pharmacologic characteristics of current models of refractory seizures, both for adult and pediatric epilepsy. In addition, we address how the National Institute of Neurological Disorders and Stroke ( NINDS)-funded Anticonvulsant Screening Program ( ASP) is evolving to incorporate appropriate animal models in the search for molecules that might be sufficiently novel to warrant further pharmacologic development. We also briefly address what we believe is necessary, going forward, to achieve the goal of stopping seizures in all patients, with a call to arms for funding agencies, the pharmaceutical industry, and basic researchers. [ABSTRACT FROM AUTHOR]

Published

2013

15. Key factors in the discovery and development of new antiepileptic drugs.

Author

Bialer, Meir and White, H. Steve

Subjects

*ANTICONVULSANTS, *CENTRAL nervous system depressants, *DRUG development, *DRUG approval, *TREATMENT of epilepsy, *ANIMALS, *BIOLOGICAL models, *DRUG interactions, *DRUG resistance, *DRUG design, *EPILEPSY, *PHARMACODYNAMICS

Abstract

Since the early 1990s, many new antiepileptic drugs (AEDs) that offer appreciable advantages in terms of their favourable pharmacokinetics, improved tolerability and lower potential for drug-drug interactions have entered the market. However, despite the therapeutic arsenal of old and new AEDs, approximately 30% of patients with epilepsy still suffer from seizures. Thus, there remains a substantial need for the development of more efficacious AEDs for patients with refractory seizures. Here, we briefly review the emerging knowledge on the pathological basis of epilepsy and how it might best be used in the design of new therapeutics. We also discuss the current approach to AED discovery and highlight some of the unique features of newer models of pharmacoresistance and epileptogenesis that have emerged in recent years. [ABSTRACT FROM AUTHOR]

Published

2010

16. Developing Novel Antiepileptic Drugs: Characterization of NAX 5055, a Systemically-Active Galanin Analog, in Epilepsy Models

Author

White, H. Steve, Scholl, Erika A., Klein, Brian D., Flynn, Sean P., Pruess, Timothy H., Green, Brad R., Zhang, Liuyin, and Bulaj, Grzegorz

Subjects

ANTICONVULSANTS, DRUG development, GALANIN, CELL receptors, ANIMAL models in epilepsy research, BLOOD-brain barrier, SEIZURES (Medicine), LABORATORY mice, PREVENTION, THERAPEUTICS, ANIMAL experimentation, BIOLOGICAL models, COMPARATIVE studies, EPILEPSY, RESEARCH methodology, MEDICAL cooperation, MICE, NEUROPEPTIDES, NEUROPHYSIOLOGY, RESEARCH, EVALUATION research, PHARMACODYNAMICS

Abstract

Summary: The endogenous neuropeptide galanin and its associated receptors galanin receptor 1 and galanin receptor 2 are highly localized in brain limbic structures and play an important role in the control of seizures in animal epilepsy models. As such, galanin receptors provide an attractive target for the development of novel anticonvulsant drugs. Our efforts to engineer galanin analogs that can penetrate the blood-brain-barrier and suppress seizures, yielded NAX 5055 (Gal-B2), a systemically-active analog that maintains low nanomolar affinity for galanin receptors and displays a potent anticonvulsant activity. In this report, we show that NAX 5055 is active in three models of epilepsy: 1) the Frings audiogenic seizure-susceptible mouse, 2) the mouse corneal kindling model of partial epilepsy, and 3) the 6 Hz model of pharmacoresistant epilepsy. NAX 5055 was not active in the traditional maximal electroshock and subcutaneous pentylenetetrazol seizure models. Unlike most antiepileptic drugs, NAX 5055 showed high potency in the 6 Hz model of epilepsy across all three different stimulation currents; i.e., 22, 32 and 44 mA, suggesting a potential use in the treatment of pharmacoresistant epilepsy. Furthermore, NAX 5055 was found to be biologically active after intravenous, intraperitoneal, and subcutaneous administration, and efficacy was associated with a linear pharmacokinetic profile. The results of the present investigation suggest that NAX 5055 is a first-in-class neurotherapeutic for the treatment of epilepsy in patients refractory to currently approved antiepileptic drugs. [Copyright &y& Elsevier]

Published

2009

17. Discovery of Antiepileptic Drugs

Author

Smith, Misty, Wilcox, Karen S., and White, H. Steve

Subjects

ANTICONVULSANTS, DRUGS, DRUG development, SPASMS, PATIENTS, ANIMAL models in research, ANIMALS, DRUG design, CLINICAL drug trials

Abstract

Summary: Since 1993, the Anticonvulsant Drug Development Program has contributed to the successful development of nine clinically effective drugs for the symptomatic treatment of epilepsy. These include felbamate (1993), gabapentin (1994), lamotrigine (1994), fosphenytoin (1996), topiramate (1996), tiagabine (1997), levetiracetam (1999), zonisamide (2000), and oxcarbazepine (2000). Despite the apparent success of the current discovery process, a significant need persists for more efficacious and less toxic antiepileptic drugs (AEDs). This is particularly true for patients whose seizures remain refractory to the currently available AEDs. This chapter will review the current process for AED discovery employed by the Anticonvulsant Drug Development Program at the University of Utah and other laboratories working toward the common goal of discovering better therapeutic options for patients living with epilepsy. It will discuss some of the inherent advantages and limitations of the primary animal models employed, while offering insight into potential future directions as we seek to better understand the pathophysiology underlying acquired epilepsy, therapy resistance, and epileptogenesis. [Copyright &y& Elsevier]

Published

2007

18. How Clinical Development Can, and Should, Inform Translational Science.

Author

Barker-Haliski, Melissa, Friedman, Daniel, White, H. Steve, and French, Jacqueline A.

Subjects

*CENTRAL nervous system diseases, *THERAPEUTICS, *TRANSLATIONAL research, *BIOMARKERS, *DRUG development, *CLINICAL trials, *PATIENTS

Abstract

There is an urgent need for preclinical translational efforts to be realized as breakthroughs in therapy for the many patients with life-altering conditions affecting the CNS. Despite intensive efforts, few transformative therapies have emerged, and many new potential therapies that looked promising in preclinical development have failed in the clinic. In this Perspective, we suggest that if preclinical scientists partner early with clinical scientists, they can begin to envision the pathway forward for their work through clinical trials. Options might include determining the populations to be treated, issues of dose selection, timing of intervention, duration of intervention, and the availability of biomarkers. In addition, understanding other factors that impact the likelihood that a proof-of-concept trial can be performed, as well as other critical issues, will altogether increase the attractiveness of the project to investors and partners and will also increase the likelihood that the intervention will succeed in the clinic. [ABSTRACT FROM AUTHOR]

Published

2014

19. Blockade of the IL-1R1/TLR4 pathway mediates disease-modification therapeutic effects in a model of acquired epilepsy.

Author

Iori, Valentina, Iyer, Anand M., Ravizza, Teresa, Beltrame, Luca, Paracchini, Lara, Marchini, Sergio, Cerovic, Milica, Hill, Cameron, Ferrari, Mariella, Zucchetti, Massimo, Molteni, Monica, Rossetti, Carlo, Brambilla, Riccardo, Steve White, H., D'Incalci, Maurizio, Aronica, Eleonora, and Vezzani, Annamaria

Subjects

*TREATMENT effectiveness, *TREATMENT of epilepsy, *INTERLEUKIN-1 receptors, *TARGETED drug delivery, *DRUG development

Abstract

We recently discovered that forebrain activation of the IL-1 receptor/Toll-like receptor (IL-1R1/TLR4) innate immunity signal plays a pivotal role in neuronal hyperexcitability underlying seizures in rodents. Since this pathway is activated in neurons and glia in human epileptogenic foci , it represents a potential target for developing drugs interfering with the mechanisms of epileptogenesis that lead to spontaneous seizures. The lack of such drugs represents a major unmet clinical need. We tested therefore novel therapies inhibiting the IL-1R1/TLR4 signaling in an established murine model of acquired epilepsy. We used an epigenetic approach by injecting a synthetic mimic of micro(mi)RNA-146a that impairs IL1R1/TLR4 signal transduction, or we blocked receptor activation with antiinflammatory drugs. Both interventions when transiently applied to mice after epilepsy onset, prevented disease progression and dramatically reduced chronic seizure recurrence, while the anticonvulsant drug carbamazepine was ineffective. We conclude that IL-1R1/TLR4 is a novel potential therapeutic target for attaining disease-modifications in patients with diagnosed epilepsy. [ABSTRACT FROM AUTHOR]

Published

2017

20. Progress report on new antiepileptic drugs: A summary of the Twelfth Eilat Conference (EILAT XII).

Author

Bialer, Meir, Johannessen, Svein I., Levy, René H., Perucca, Emilio, Tomson, Torbjörn, and White, H. Steve

Subjects

*ANTICONVULSANTS, *TREATMENT of epilepsy, *DRUG development, *CLINICAL pharmacology, *CLINICAL pharmacologists, *SCIENTISTS, *NEUROLOGISTS

Abstract

Summary The Twelfth Eilat Conference on New Antiepileptic Drugs (AEDs) – EILAT XII, took place in Madrid, Spain from August 31st to September 3rd 2014. About 130 basic scientists, clinical pharmacologists and neurologists from 22 countries attended the conference, whose main themes included “Conquering pharmacoresistant epilepsy”, “Innovative emergency treatments”, “Progress report on second-generation treatment” and “New methods and formulations”. Consistent with previous formats of this conference, a large part of the program was devoted to a review of AEDs in development, as well as updates on AEDs introduced since 2004. Like the EILAT X and EILAT XI reports, the current article focuses on the preclinical and clinical pharmacology of AEDs that are currently in development. These include adenosine-releasing silk, allopregnanolone (SAGE-547), AMP-X-0079, brivaracetam, bumetanide, cannabidiol, cannabidivarin, 2-deoxy-glucose, everolimus, ganaxolone, huperzine A, imepitoin, minocycline, NAX 801-2, pitolisant, PRX 0023, SAGE-217, valnoctamide and its homologue sec -butyl-propylacetamide (SPD), and VLB-01. Since the previous Eilat conference, perampanel has been introduced into the market and twelve novel potential epilepsy treatments are presented for the first time. [ABSTRACT FROM AUTHOR]

Published

2015

21. Progress report on new antiepileptic drugs: A summary of the Eleventh Eilat Conference (EILAT XI)

Author

Bialer, Meir, Johannessen, Svein I., Levy, René H., Perucca, Emilio, Tomson, Torbjörn, and White, H. Steve

Subjects

*ANTICONVULSANTS, *CONFERENCES & conventions, *SCIENTISTS, *CLINICAL pharmacologists, *NEUROLOGISTS, EPILEPSY research

Abstract

Summary: The Eleventh Eilat Conference on New Antiepileptic Drugs (AEDs)-EILAT XI, took place in Eilat, Israel from the 6th to 10th of May 2012. About 100 basic scientists, clinical pharmacologists and neurologists from 20 countries attended the conference, whose main themes included “Indications overlapping with epilepsy” and “Securing the successful development of an investigational antiepileptic drug in the current environment”. Consistent with previous formats of this conference, a large part of the program was devoted to a review of AEDs in development, as well as updates on AEDs introduced since 1994. Like the EILAT X report, the current manuscript focuses only on the preclinical and clinical pharmacology of AEDs that are currently in development. These include brivaracetam, 2-deoxy-glucose, ganaxolone, ICA-105665, imepitoin, NAX 801-2, perampanel and other AMPA receptor antagonists, tonabersat, valnoctamide and its homologue sec-propylbutylacetamide (SPD), VX-765 and YK3089. Since the previous Eilat conference, retigabine (ezogabine) has been marketed and four newer AEDs in development (NAX 810-2, SPD, tonabersat and VX-765) are included in this manuscript. [Copyright &y& Elsevier]

Published

2013

22. Progress report on new antiepileptic drugs: A summary of the Tenth Eilat Conference (EILAT X)

Author

Bialer, Meir, Johannessen, Svein I., Levy, René H., Perucca, Emilio, Tomson, Torbjörn, and White, H. Steve

Subjects

*ANTICONVULSANTS, *CLINICAL pharmacologists, *NEUROLOGISTS, *CLINICAL pharmacology, *ANIMAL models in research, *DRUG development, *CLINICAL trials, *EPILEPSY

Abstract

Summary: The Tenth Eilat Conference on New Antiepileptic Drugs (AEDs)-EILAT X, took place in Eilat, Israel from the 25th to 29th of April 2010. About 200 basic scientists, clinical pharmacologists and neurologists from 25 countries attended the conference, whose main themes included learning from the past: Lessons learnt after 18 years of Eilat Conferences and Detecting assessing and preventing adverse effects of AEDs. Consistent with previous formats of this conference, a large part of the program was devoted to a review of AEDs in development, as well as updates on AEDs introduced since 1994. Like the previous EILAT (EILAT IX) manuscript, the current (EILAT X) manuscript focuses only on the preclinical and clinical pharmacology of AEDs that are currently in development. These include brivaracetam, carisbamate, 2-deoxy-glucose, ganaxolone, huperizine A, ICA-105665, NAX-5055, retigabine, perampanel, T-2007, valnoctamide and YK3089. Since the previous Eilat Conference (EILAT IX-2008) two new AEDs; eslicarbazepine acetate and lacosamide have been marketed and three new AEDs in development not included in the EILAT IX manuscript were added: ICA-105665, perampanel and valnoctamide. The CNS efficacy of these compounds in anticonvulsant animal models as well as other disease model systems are presented in and their proposed mechanism of action at summarized in . [ABSTRACT FROM AUTHOR]

Published

2010

23. Progress report on new antiepileptic drugs: A summary of the Ninth Eilat Conference (EILAT IX)

Author

Bialer, Meir, Johannessen, Svein I., Levy, René H., Perucca, Emilio, Tomson, Torbjörn, and White, H. Steve

Subjects

*ANTICONVULSANTS, *DRUG development, *TARGETED drug delivery, *CLINICAL pharmacologists, *CONFERENCES & conventions, *TREATMENT of epilepsy, *CLINICAL trials

Abstract

Summary: The Ninth Eilat Conference on New Antiepileptic Drugs (AEDs)-EILAT IX, took place in Sitges, Barcelona from the 15th to 19th of June 2008. Over 300 basic scientists, clinical pharmacologists and neurologists from 25 countries attended the conference, whose main themes included old and new AEDs in generalized epilepsies, novel formulations and routes of administration of AEDs, common targets and mechanisms of action of drugs for treating epilepsy and other central nervous system (CNS) disorders, and opportunities and perspectives in new AED discovery. Consistent with previous formats of this conference, a large part of the programme was devoted to a review of AEDs in development, as well as updates on AEDs introduced since 1989. Unlike previous EILAT manuscripts, the current (EILAT IX) manuscript focuses only on the preclinical and clinical pharmacology of AEDs that are currently in development. These include brivaracetam, carisbamate (RWJ-333369), 2-deoxy-d-glucose, eslicarbazepine acetate (BIA-2-093), ganaxolone, huperzine, JZP-4, lacosamide, NAX-5055, propylisopropylacetamide (PID), retigabine, T-2000, tonabersat, valrocemide and YKP-3089. The CNS efficacy of these compounds in anticonvulsant animal models as well as other disease model systems are presented in first and second tables and their proposed mechanisms of action are summarized in the third table. [Copyright &y& Elsevier]

Published

2009