grant

Neurological Disorders in HIV-1 Infection

Organization UNIVERSITY OF NEBRASKA MEDICAL CENTERLocation OMAHA, UNITED STATESPosted 15 Aug 2024Deadline 30 Jun 2026
NIHUS FederalResearch GrantFY20252-oxo-propanalAD dementiaAIDS VirusAcetylformaldehydeAcquired Immune Deficiency Syndrome VirusAcquired Immunodeficiency Syndrome VirusAdeno-Associated VirusesAdhesionsAlzheimer Type DementiaAlzheimer disease dementiaAlzheimer sclerosisAlzheimer syndromeAlzheimer'sAlzheimer's DiseaseAlzheimers DementiaAmmon HornAnti-Retroviral AgentsAnxietyArginineAssayAstrocytesAstrocytusAstrogliaAttentionAttentional deficitAttenuatedAxonBehaviorBioassayBiological AssayBiologyBlood PlasmaBlood VesselsBrainBrain Nervous SystemBrain regionCNS DiseasesCNS disorderCardiovascular DiseasesCell BodyCell LineCellLineCellsCentral Nervous System DiseasesCentral Nervous System DisordersCornu AmmonisCyclic PeptidesCyclicityDarknessDataDendritesDependoparvovirusDependovirusDevelopmentDiseaseDisorderDrug TherapyDrugsEPSPElectrophysiologyElectrophysiology (science)EncephalonEndotheliumEnzyme GeneEnzymesExcitatory Postsynaptic PotentialsExhibitsExtravasationFrequenciesFumaratesGene TransferGenus HippocampusGlycolysisGlyoxalase IHIVHIV InfectionsHIV-1HIV-IHIV1HTLV-III InfectionsHTLV-III-LAV InfectionsHarvestHippocampusHortega cellHumanHuman Immunodeficiency Virus Type 1Human Immunodeficiency VirusesHuman T-Lymphotropic Virus Type III InfectionsHuman immunodeficiency virus 1ImpairmentIncidenceInfectionInflammationIntermediary MetabolismL-ArginineLAV-HTLV-IIILactoyl Glutathione LyaseLactoylglutathione LyaseLeakageLearningLightLinkLymphadenopathy-Associated VirusMeasuresMediatingMedicationMemoryMetabolic ProcessesMetabolismMethylglyoxalMethylglyoxalaseMiceMice MammalsMicrogliaModern ManMolecularMovementMsecMurineMusNerve CellsNerve UnitNervous System DiseasesNervous System DisorderNervous System PhysiologyNeural CellNeural TransmissionNeurocyteNeurodevelopmental DisorderNeurologic DisordersNeurologic functionNeurological Development DisorderNeurological DisordersNeurological functionNeuronsNeurophysiology / ElectrophysiologyOlder PopulationOutputPeptidesPerformancePeriodicityPersonsPharmaceutical PreparationsPharmacological TreatmentPharmacotherapyPhotoradiationPhysiologic pulsePlasmaPlasma SerumPrimary Senile Degenerative DementiaProteinsProtocolProtocols documentationPulsePyruvaldehydePyruvic AldehydeReactionRegimenReportingReticuloendothelial System, Serum, PlasmaRhythmicitySeahorseSliceSpillageStrains Cell LinesStructure-Activity RelationshipSymptomsSynapsesSynapticSynaptic TransmissionTenofovirTestingThalamic structureThalamusTimeUniversitiesUpregulationVireadVirus-HIVadeno associated virus groupaged groupaged groupsaged individualaged individualsaged peopleaged personaged personsaged populationaged populationsaging populationanti-retroviralantiretroviral therapyantiretroviral treatmentastrocytic gliaattentive deficitattenuateattenuatesbeta-L-2',3'-dideoxy-5-fluoro-3'-thiacytidinebody movementcardiovascular disordercell typechemical structure functionclinical relevanceclinically relevantco-morbidco-morbiditycomorbiditycultured cell linecytotoxicdetermine efficacydevelopmentaldrug interventiondrug treatmentdrug/agentearly onsetefficacy analysisefficacy assessmentefficacy determinationefficacy evaluationefficacy examinationelectrophysiologicalemtricitabineevaluate efficacyexamine efficacyfeedingfield based datafield learningfield studyfield testgitter cellglyoxalasehippocampalhumanized micehumanized mousein vivoinflammation markerinflammatory markerinsightmesogliamicroglial cellmicrogliocytemid lifemid-lifemiddle agemiddle agedmidlifemillisecondmouse modelmurine modelnervous system functionneurodevelopmental diseaseneurological diseaseneuronalnovelobject recognitionolder groupsolder individualsolder personperivascular glial cellpharmaceutical interventionpharmacological interventionpharmacological therapypharmacology interventionpharmacology treatmentpharmacotherapeuticspopulation agingprepulse inhibitionprimary degenerative dementiaprocessing speedresponsesenile dementia of the Alzheimer typesexstructure function relationshipsynapsethalamicvascularvascular inflammation
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Full Description

ABSTRACT
There is a high incidence of neurological disorders (HAND) in middle-aged people living with HIV infection

(PLWH). To date, the molecular causes for diverse array of HAND remain poorly understood, and specific

pharmacological interventions to manage HAND remain elusive. The working hypothesis for this R21 is “that

the reactive glycolytic byproduct methylglyoxal (MG) is triggering the multitude of early-onset neurological

disorders by exerting varying actions of different cell types in the brain”. The aims are (1) define pathobiological

trajectory of early-onset neurological disorders in relation to MG, Glo-1, microvascular leakage, and inflammation

in HIV-1 infected Hu-mice with and with anti-retroviral treatment, and (2) show that lowering MG with novel, cell-

penetrant arginine-rich cyclic peptides will blunt neurological disorders in HIV-infected Hu-mice with and without

anti-retroviral treatment. Data generated from this R21 will establish for the first time a link between the elevated

levels of the glycolysis byproduct MG, microvascular leakage, impaired synaptic transmission, and neurological

disorders, in our clinically relevant HIV-1 infected Hu-mice model. Preliminary structure-activity relationship

studies will also provide novel insights into the use of arginine-rich cyclic peptides to scavenge MG and attenuate

these early-onset HAND.

Grant Number: 5R21NS139920-02
NIH Institute/Center: NIH

Principal Investigator: KESHORE BIDASEE

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