grant

Novel hybrid molecule with both IOP lowering and neuroprotective effects for treatment of glaucoma

Organization UNIVERSITY OF NORTH TEXAS HLTH SCI CTRLocation FORT WORTH, UNITED STATESPosted 1 Sept 2020Deadline 31 Aug 2026
NIHUS FederalResearch GrantFY202421+ years old3-mononitrotyrosine3-nitrotyrosineActive OxygenAddressAdultAdult HumanAffectAfrican Green MonkeyAfter CareAfter-TreatmentAftercareAllergic ReactionAnimal ModelAnimal Models and Related StudiesAnteriorAntioxidantsApoptoticAqueous HumorAutoregulationBilateralBioavailabilityBiochemicalBiological AvailabilityBlindnessBody TissuesBone-Derived Transforming Growth FactorBrimodineCell BodyCell DeathCell ProtectionCell SurvivalCell ViabilityCell-Extracellular MatrixCellsCessation of lifeCharacteristicsChlorocebus aethiopsChlorocebus sabaeusChronicClinicalClinical TrialsCollaborationsCommon Rat StrainsCorneal DiseasesCorneal DisorderCranial Nerve IICytoprotectionDeathDegenerative Neurologic DisordersDiseaseDisorderDoppler OCTDoseDrug KineticsECMElectroretinographyEncapsulatedEndogenous Nitrate VasodilatorEndothelium-Derived Nitric OxideEstersExtracellular MatrixEyeEye DropsEye diseasesEyeballEyedropsFDA approvedFormulationFree RadicalsFrequenciesFutureGene ExpressionGlaucomaGlobal ChangeGoalsGreen MonkeyHomeostasisHumanHybridsHypoxiaHypoxicInjuryIntraocular FluidIntraocular PressureLaser ElectromagneticLaser RadiationLasersLatanoprostLipid PeroxidationMeasuresMediatingMercaptansMercapto CompoundsMethodsMiceMice MammalsMilk Growth FactorModelingModern ManMonkeysMononitrogen MonoxideMurineMusNO3-NatureNerve CrushNervous System Degenerative DiseasesNeural Degenerative DiseasesNeural degenerative DisordersNeurodegenerative DiseasesNeurodegenerative DisordersNeurologic Degenerative ConditionsNitratesNitric OxideNitric Oxide DonorsNitrogen MonoxideNitrogen ProtoxideOCT TomographyOcular HypertensionOcular TensionOptic NerveOptical Coherence TomographyOxygen DeficiencyOxygen RadicalsPG AnalogsPOAGPathologyPathway interactionsPatientsPatternPersonsPharmacokineticsPhysiologic AvailabilityPhysiologic Intraocular PressurePhysiological HomeostasisPlatelet Transforming Growth FactorPosterior Eye SegmentPosterior eyeball segment structurePredispositionPrevalencePrimary Open Angle GlaucomaPro-OxidantsProductionProstaglandin AnalogsRNA SeqRNA sequencingRNAseqRatRats MammalsRattusReactive Oxygen SpeciesRegulationRelaxationRetinaRetinal Ganglion CellsRodentRodent ModelRodentiaRodents MammalsRouteSafetySecond Cranial NerveSulfhydryl CompoundsSusceptibilitySuspension substanceSuspensionsSynthetic ProstaglandinsSystemTGF BTGF-betaTGF-βTGFbetaTGFβTestingTherapeuticThiolsTissuesTopical Drug AdministrationTopical applicationToxicokineticsTrabecular MeshworkTrabecular meshwork structureTransforming Growth Factor betaTransforming Growth Factor-Beta Family GeneTraumatic injuryVenous Blood PressureVenous PressureVenous Pressure leveladminister topicallyadulthoodage associated declineage dependent declineage related declinealpha 2 agonistanti-oxidant enzymeantioxidant enzymeapply topicallyaqueousaxonal degenerationblindbrimonidinebromoxidinecornea disordercytoprotectivedecline with agedegenerative axondegenerative diseases of motor and sensory neuronsdegenerative neurological diseasesdeliver topicallydelivery vectordelivery vehicledetermine efficacydrug release profileefficacy analysisefficacy assessmentefficacy determinationefficacy evaluationefficacy examinationelectroretinogramendothelial cell derived relaxing factorevaluate efficacyexamine efficacyeye disordereye toxicityfunctional groupglaucomatousin vivoinjuriesintra-ocular pressureintravitreal injectionmimeticsmodel of animalmouse modelmurine modelnano particlenano polymernano-sized particlenanoparticlenanoparticle drugnanopolymernanosized particlenecrocytosisneurodegenerative illnessneuroprotectionneuroprotectivenew drug treatmentsnew drugsnew pharmacological therapeuticnew therapeuticsnew therapynext generation therapeuticsnitratenitrotyrosinenormotensivenovelnovel drug treatmentsnovel drugsnovel pharmaco-therapeuticnovel pharmacological therapeuticnovel therapeuticsnovel therapyocular diseaseocular disorderocular hypertensiveocular toxicityophthalmopathyoptical Doppler tomographyoptical coherence Doppler tomographypathwaypatient populationpost treatmentpreservationpressurepreventpreventingretinal ganglionretinal ganglion cell degenerationretinal toxicitysafety assessmentside effectsmall moleculestemsulfhydryl grouptopical administrationtopical deliverytopical drug applicationtopical treatmenttopically administeredtopically appliedtopically deliveredtopically treatedtranscriptome sequencingtranscriptomic sequencingtreat topicallytreatment effectvision lossvisual lossα2 agonist
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Full Description

Glaucoma is a neurodegenerative disease of the eye with an estimated prevalence of 80 million patients
worldwide by 2020, at least 6 to 8 million becoming bilaterally blind. Elevated intraocular pressure (IOP)

causing axonal degeneration of the optic nerve and progressive loss of retinal ganglion cells (RGCs)

which are the characteristic hallmarks of glaucoma. Clinically, the only method of slowing glaucomatous

vision loss is to reduce intraocular pressure (IOP), which is partially effective and doesn’t address

susceptibility to RGC degeneration. Current therapy for glaucoma includes use of prostaglandin analogs

based IOP lowering agents, however, about 10% of glaucoma patients don’t respond to these therapies.

Brimonidine, an α2 agonist, eye-drop lowers IOP and is also neuroprotective, however it causes many

side effects such as allergic reactions and corneal disorders. Along with IOP, age related decline in anti-

oxidant enzymes in ocular tissues contributes to the death of both RGCs and trabecular meshwork (TM)

cells, which is not addressed by available treatments. The nitric oxide (NO) system could potentially be

targeted to enhance the aqueous outflow by relaxing the trabecular meshwork (TM) cells to lower IOP.

Here, we propose to develop a robust hybrid NO donating and SOD mimetic compound encapsulated in

PLGA nanoparticle which will prolong the duration of lowering IOP and also have neuroprotective effects.

We have synthesized a novel bi-functional hybrid compound SA-2 with NO donor and SOD mimetic

functional groups. Our preliminary results demonstrated that, a single eye drop of PLGA encapsulated

SA-2 nanoparticles (SA-2-NPs) lowered IOP by 50% in a mouse glaucoma model. Additionally,

compound SA-2 is highly neuroprotective both in ex vivo hypoxic insult of adult rat retinal explants and

in in vivo mouse optic nerve crush model via intravitreal injection. Our goals are 1) to optimize the dose

via toxicokinetic study of SA-2-NPs and determine the efficacy to lower IOP in two animal models: a

mouse model of ocular hypertension (OHTN) induced by Ad5.TGFβ2 and in normotensive monkey eyes.

2) To delineate the biochemical mechanisms through which compound SA-2 protects both human TM

cells and RGCs from glaucomatous changes. 3) To assess the topically administered SA-2-NPs for their

ability to prevent RGC death in two models: a mouse model of optic nerve crush (traumatic injury) and a

mouse model of ocular hypertension (chronic injury). Successful completion of the above proposed

studies will provide information on the maximum effective dose of and frequency of dosing of SA-2-NPs

that will be further evaluated in laser induced OHTN monkey model as our future goal and eventually will

progress to human clinical trials. The results will have a major impact in the field with implications for

developing novel non-prostaglandin therapeutics that have both IOP lowering and neuroprotective

effects.

Grant Number: 5R01EY029823-05
NIH Institute/Center: NIH

Principal Investigator: Suchismita Acharya

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