Development of a Soluble Epoxide Hydrolase Inhibitor to Spare or Replace Opioid Analgesics
Project Number4UH3DA048767-03
Former Number4UG3DA048767-03
Contact PI/Project LeaderCORTES-PUCH, IRENE Other PIs
Awardee OrganizationEICOSIS, LLC
Description
Abstract Text
Summary/Abstract
EicOsis is developing a first-in-class analgesic with efficacy against neuropathic pain that will
replace and dose spare opioids and thus prevent opioid use disorders (OUDs). The target of the
small molecule inhibitor EC5026 is the soluble epoxide hydrolase, a master regulatory enzyme
that modulates the activity of endogenous bioactive lipids. The development of EC5026 is
currently in progress and progressing to an IND filing and is poised to have a high impact in
treating chronic pain in humans. In this proposal we outline aims to reach the next steps in
clinical human clinical trials with EC5026 as well as additional preclinical studies to expand the
efficacy into models of chronic pain conditions presenting in humans which are most frequently
treated with opioids. Additionally, we propose detailed pharmacokinetic, metabolism and
distribution studies that will provide the required information for advanced clinical trials
examining efficacy in humans. We also propose to optimize a formulation to meet these needs.
All of these individual aims are structured to meet 2 year milestones (UG3) and continue to the
next planned steps in development (UH3) as these milestones are met. EicOsis is meeting
current development goals and EC5026 is well positioned to meet the urgent need of reducing
opioid use because even given the updated strategy to treating pain with multimodal
approaches, pharmaceuticals are the foundation of treating pain. EC5026 represents a first-in-
class analgesic that is not an opioid nor a NSAID but offers effective pain relief for chronic
neuropathic pain.
Public Health Relevance Statement
Narrative
Inhibiting the soluble epoxide hydrolase enzyme offers a potent, first-in-class analgesic strategy
to treat chronic neuropathic pain conditions while replacing and dose reducing the use of
opioids. EicOsis is moving the IND candidate EC5026 rapidly to market as a safe, effective and
non-addictive strategy to treat chronic pain. Preclinical results with EC5026 show broad efficacy
in neuropathic models and preparation for an IND filing is underway, here we continue the drive
to clinical trials in humans.
NIH Spending Category
No NIH Spending Category available.
Project Terms
AccidentsAnalgesicsAttenuatedBiochemicalBiologicalBiological MarkersCanis familiarisCessation of lifeChemicalsClinicalClinical TrialsCombined Modality TherapyCyclic GMPDataDevelopmentDoseDrug KineticsEnsureEnzymesEpoxide hydrolaseFastingFatty AcidsFormulationFoundationsGoalsHumanIndividualLipidsLow Back PainMarketingMedicineMetabolismModelingMonitorMorbidity - disease rateNational Institute of Neurological Disorders and StrokeNeuropathyNon-Steroidal Anti-Inflammatory AgentsOpioidOpioid AnalgesicsPainPain managementPatientsPharmacologic SubstancePhasePhase Ia TrialPolyunsaturated Fatty AcidsPositioning AttributePreparationRattusRefractoryRodentSafetySamplingSpinal cord injurySpinal cord injury patientsStructureTestingTherapeutic EquivalencyTreatment EfficacyUnited StatesUnited States National Institutes of HealthUpdateWorkaddictionbehavioral outcomecapsulechronic neuropathic painchronic pain managementchronic pain reliefchronic painful conditionclinical developmentcomparative efficacydesignefficacy evaluationefficacy studyefficacy testingefficacy trialhuman subjectinflammatory paininhibitorlead candidatemanufacturemeetingsmortalitymultimodalitynovelopioid overdoseopioid sparingopioid useopioid use disorderpain modelpain reliefpainful neuropathypatient populationphase 2 designspre-clinicalpreclinical efficacypreclinical safetypreclinical studyprescription opioidpreventprogramssafety assessmentsafety studysafety testingside effectsmall molecule inhibitor
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