SBIR-STTR Award

Extended Neuroamides: Novel Antiepileptic Drug Candidates
Award last edited on: 4/3/19

Sponsored Program
STTR
Awarding Agency
NIH : NINDS
Total Award Amount
$248,926
Award Phase
1
Solicitation Topic Code
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Principal Investigator
Harold Kohn

Company Information

Neurogate Therapeutics Inc

2500 Wachovia Capitol 150 Fayetteville Street
Raleigh, NC 27601
   (919) 843-8112
   N/A
   N/A

Research Institution

Indiana University - Purdue

Phase I

Contract Number: 1R41NS080278-01
Start Date: 9/28/12    Completed: 8/31/13
Phase I year
2012
Phase I Amount
$248,926
Epilepsy is a set of disorders that result from neuronal hyperexcitability and hypersynchronous neuronal firing. Epilepsy remains a major widespread neurological concern. Current medications do not meet the health needs of 30% of epilepsy patients, and approximately 40% of patients experience serious side effects. So, the need for novel, more effective therapies is apparent. NeuroGate Therapeutics (NGT) has advanced a novel class of agents termed Extended NeuroAmides (ENAs), which have exhibited, in established animal seizure models, superb anticonvulsant activities comparable or better than most antiepileptic drugs. Recent studies have documented that the sodium channel slow inactivation (SI) state is a valid target for epilepsy. NGT has demonstrated that ENAs preferentially, potently, and stereospecifically transition Na+ channels into the SI state, and show frequency (use)-dependency. ENA Na+ channel SI activity far exceeded that of any reported anticonvulsant agent. These findings indicated that ENAs can reduce the pathological activity associated with neuronal hyperexcitability (sustained depolarization, high-frequency spiking) without significantly disrupting normal physiological activity. ENAs have shown no interactions with receptors known to adversely impact drug effectiveness. In this proposal, NGT requests funds to identify the optimal ENA that would permit investigational new drug (IND)-enabling studies in the STTR phase II grant. In Specific Aim 1, NGT will build upon an evolving structure-activity relationship study using synthesis, whole animal pharmacology that determines efficacy and neurotoxicity, and CAD cell patch-clamp electrophysiology to identify ENAs of interest. Four selected ENAs will be tested for CYP-450 inhibition and evaluated by electrophysiology using hippocampal cells. In Specific Aim 2, NGT will evaluate the two most promising ENAs in recombinant cell lines that express CNS Na+ channels (NaV1.1, NaV1.2, NaV1.3, NaV1.6) and cardiac NaV1.5 channel in order to gain information on mechanism of action and safety. In Specific Aim 3, NGT will evaluate the bioavailability in the rat of the most promising ENA and the utility of this ENA for treating pharmacoresistant epilepsy. Identifying an optimized ENA for the IND-enabling studies will permit NGT to advance a compound for clinical testing, with the support of phase II STTR funding.

Public Health Relevance:
Epilepsy is a serious neurological disorder that affects 1% of the world population and for which current medications are ineffective for 30% of patients. We have identified a new class of compounds, termed Extended NeuroAmides, that exhibit potent activities in established anticonvulsant animal models and that function by a unique mechanism of action. The proposed investigation provides a critical path for ENA development and selection allowing for IND- enabling studies in the STTR phase II study.

Public Health Relevance Statement:
Epilepsy is a serious neurological disorder that affects 1% of the world population and for which current medications are ineffective for 30% of patients. We have identified a new class of compounds, termed Extended NeuroAmides, that exhibit potent activities in established anticonvulsant animal models and that function by a unique mechanism of action. The proposed investigation provides a critical path for ENA development and selection allowing for IND- enabling studies in the STTR phase II study.

NIH Spending Category:
Brain Disorders; Epilepsy; Neurodegenerative; Neurosciences

Project Terms:
Adverse effects; Affect; Amino Acids; Animal Model; Animals; Anticonvulsants; Antiepileptic Agents; Back; Biological Assay; Biological Availability; Brain; Cardiac; Cell Line; Cell model; Cells; Cerebral hemisphere structure (body structure); Cessation of life; cost; Country; Critical Pathways; Dependency (Psychology); Development; Diagnosis; Disease; Dizziness; Drowsiness; drug candidate; drug market; effective therapy; Effectiveness; Electroconvulsive Shock; Electrophysiology (science); Epilepsy; Exhibits; experience; Frequencies (time pattern); Funding; Generations; Genetic; Grant; Health; Hippocampus (Brain); improved; Injury; interest; Investigation; Investigational Drugs; Investigational New Drug Application; Laboratories; Legal patent; Medical; meetings; Modeling; Nausea; nervous system disorder; Neurologic; Neurons; neurotoxicity; North Carolina; novel; painful neuropathy; Parkinson Disease; patch clamp; Pathway interactions; Patient Care; Patients; Pharmaceutical Preparations; Pharmacology; Phase; phase 2 study; Physiological; Population; pre-clinical; preclinical study; premature; Property; Quality of life; Rattus; receptor; Recombinants; Reporting; research clinical testing; Risk; Safety; SCN2A protein; Seizures; Small Business Technology Transfer Research; Sodium Channel; Specificity; Structure-Activity Relationship; Testing; Therapeutic; Universities; voltage

Phase II

Contract Number: ----------
Start Date: 00/00/00    Completed: 00/00/00
Phase II year
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Phase II Amount
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