grant

Investigating the role of Wnt signaling effectors on the neuron-glia switch and OPC specification during development and after injury.

Organization UNIVERSITY OF COLORADO DENVERLocation Aurora, UNITED STATESPosted 1 Jan 2024Deadline 30 Nov 2026
NIHUS FederalResearch GrantFY2025AffectAxonBasal Transcription FactorBasal transcription factor genesBindingBinding SitesBrachydanio rerioCRISPR approachCRISPR based approachCRISPR methodCRISPR methodologyCRISPR techniqueCRISPR technologyCRISPR toolsCRISPR-CAS-9CRISPR-based methodCRISPR-based techniqueCRISPR-based technologyCRISPR-based toolCRISPR/CAS approachCRISPR/Cas methodCRISPR/Cas technologyCRISPR/Cas9CRISPR/Cas9 technologyCas nuclease technologyCell BodyCell Communication and SignalingCell SignalingCellsChromatinClustered Regularly Interspaced Short Palindromic Repeats approachClustered Regularly Interspaced Short Palindromic Repeats methodClustered Regularly Interspaced Short Palindromic Repeats methodologyClustered Regularly Interspaced Short Palindromic Repeats techniqueClustered Regularly Interspaced Short Palindromic Repeats technologyCombining SiteDanio rerioDataDevelopmentDoseFailureGene ExpressionGene TranscriptionGeneral Transcription Factor GeneGeneral Transcription FactorsGenerationsGenesGeneticGenetic TranscriptionGenetics-MutagenesisGliaGlial CellsGlial DifferentiationImageImaging ProceduresImaging TechnicsImaging TechniquesImmunohistochemistryImmunohistochemistry Cell/TissueImmunohistochemistry Staining MethodInjuryIntracellular Communication and SignalingKolliker's reticulumLarvaMammaliaMammalsMapsMediatorMedulla SpinalisMolecularMolecular InteractionMotor CellMotor NeuronsMutagenesisMutagenesis Molecular BiologyNatural regenerationNerve CellsNerve UnitNervous System DiseasesNervous System DisorderNeural CellNeural Stem CellNeurocyteNeurogliaNeuroglial CellsNeurologic DisordersNeurological DisordersNeuronal DifferentiationNeuronsNon-neuronal cellNonneuronal cellOligodendrocytesOligodendrocytusOligodendrogliaOligodendroglia CellPositionPositioning AttributePostdocPostdoctoral FellowProcessProductionProgenitor CellsRNA ExpressionReactive SiteRegenerationRegulationResearch AssociateRoleSignal TransductionSignal Transduction SystemsSignalingSourceSpecific qualifier valueSpecifiedSpinal CordSpinal Cord TraumaSpinal TraumaSpinal cord injuredSpinal cord injurySupporting CellTechniquesTestingTrainingTranscriptTranscriptionTranscription Factor Proto-OncogeneTranscription factor genesTransgenic OrganismsTraumatic MyelopathyVertebrate AnimalsVertebratesVisualizationWNT Signaling PathwayWNT signalingZebra DanioZebra FishZebrafishbiological signal transductiondevelopmentalexperimentexperimental researchexperimental studyexperimentsfunctional restorationgain of functiongene regulatory networkglial cell developmentglial developmentgliogenesisgraduate studentimage-based methodimagingimaging methodimaging modalityin vivoinjuriesinjury recoveryinsightloss of functionmotoneuronmultiomicsmultiple omicsmyelinationnerve cementnerve stem cellnervous system developmentneural circuitneural circuitryneural precursorneural precursor cellneural progenitorneural progenitor cellsneural stem and progenitor cellsneurocircuitryneurogenesisneurogenic progenitorsneurogenic stem cellneurological diseaseneuron progenitorsneuronalneuronal progenitorneuronal progenitor cellsneuronal stem cellsneuronal survivalneuroprogenitoroligodendrocyte lineageoligodendrocyte precursoroligodendrocyte precursor celloligodendrocyte progenitoroligodendrocyte stem cellpanomicspharmacologicpost-docpost-doctoralpost-doctoral traineeprogenitorprogenitor and neural stem cellsprogenitor cell differentiationprogenitor cell fate specificationprogenitor cell poolprogenitor cell populationprogenitor cell proliferationprogenitor differentiationprogenitor fate specificationprogenitor poolprogenitor populationprogenitor proliferationprogenitor specificationrecovery after injuryrecovery following injuryrecovery post injuryregenerateregenerativeresearch associatesresponserestore functionrestore functionalityrestore lost functionscRNA sequencingscRNA-seqsingle cell RNA-seqsingle cell RNAseqsingle cell expression profilingsingle cell transcriptomic profilingsingle-cell RNA sequencingsocial rolestem and progenitor cell populationstem and progenitor cell proliferationstem and progenitor differentiationstem cell differentiationstem cell fate specificationstem cell poolstem cell populationstem cell proliferationstem cell specificationstem cellssynaptic circuitsynaptic circuitrytooltranscription factortransgenicvertebrata
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Full Description

PROJECT SUMMARY
Nervous system development and regeneration relies on sequential and coordinated formation of diverse
neurons and glia from neural progenitor cells. Though neuronal and glial differentiation is extensively studied,
less is known about the molecular signals that modulate the transition from neurogenesis to gliogenesis.
Oligodendrocytes, glial cells that support axon conduction and survival through myelination, are essential for
nervous system development and regeneration. During spinal cord development, distinct neural progenitors in
the pMN domain undergo a neuron-glia switch to sequentially produce motor neurons followed by
oligodendrocyte progenitor cells (OPCs). Similarly, successful regeneration after spinal cord injury requires the
coordinated production of both neurons and oligodendrocytes to functionally restore damaged circuits. Zebrafish
are highly regenerative compared to mammals and endogenous neural progenitors produce motor neurons after
injury, but interestingly do not produce OPCs. The molecular mechanisms that regulate the neuron-glia switch
to specify neural progenitor cells into a neuronal or oligodendrocyte fate during development and after injury
remain unknown. Recently, our lab conducted fate mapping and single-cell RNAseq and revealed a molecularly
distinct subset of pMN neural progenitors, pre-OPCs, that are specified to commit to the oligodendrocyte lineage.
Our data revealed that pre-OPCs are uniquely enriched for factors involved in Wnt signaling, a cascade that
modulates OPC differentiation during development and that is reactivated after injury to regulate neurogenesis.
Using zebrafish, I will utilize immunohistochemistry and transgenic imaging techniques alongside CRISPR/Cas9
mutagenesis strategies to determine how axin1 modulates wnt expression in pMN progenitors to activate a
transcriptional switch in tcf7l2 and drive a neuron-glia switch to specify pMN progenitor cells into pre-OPCs.
Further, through powerful single-cell multi-omics techniques I will identify transcriptional interactions with
neuronal and oligodendrocyte-specific genes in pMN progenitors to establish a gene regulatory network that
drives the neuron-glia switch. Finally, I will use pharmacological and genetic tools to manipulate wnt expression
after spinal cord injury and induce a neuron-glia switch in vivo to drive gliogenesis in endogenous neural
progenitor cells. Together, these studies will uncover molecular regulators of pMN progenitor specification and
highlight the role of the neuron-glia switch in nervous system development and regeneration.

Grant Number: 5F32NS134612-02
NIH Institute/Center: NIH
Principal Investigator: Kimberly Arena

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