grant

Uncovering brain-wide molecular determinants of individual memory performance across lifespan

Organization BAYLOR COLLEGE OF MEDICINELocation HOUSTON, UNITED STATESPosted 15 Sept 2022Deadline 31 Aug 2027
NIHUS FederalResearch GrantFY2025AD dementiaAgeAge associated cognitive deficitAge associated cognitive dysfunctionAge related memory declineAge related memory deficitAge related memory impairmentAge-associated cognitive declineAge-related cognitive declineAgingAlzheimer Type DementiaAlzheimer disease dementiaAlzheimer sclerosisAlzheimer syndromeAlzheimer'sAlzheimer's DiseaseAlzheimers DementiaBehaviorBehavioralBenign senescent forgetfulnessBrainBrain Nervous SystemBrain regionC elegansC. elegansC.elegansCaenorhabditis elegansComplexDiseaseDisorderEncephalonExhibitsGenomicsHumanIndividualInvertebrataInvertebratesLearningMemoryMemory LossModelingModern ManMolecularNerve CellsNerve UnitNervous SystemNervous System DiseasesNervous System DisorderNervous System PhysiologyNeural CellNeurocyteNeurodevelopmental DisorderNeurologic Body SystemNeurologic DisordersNeurologic Organ SystemNeurologic functionNeurological Development DisorderNeurological DisordersNeurological functionNeuronsNeurosciencesOrganismPathway interactionsPerformancePhysiologicPhysiologicalPrimary Senile Degenerative DementiaProcessSynapsesSynapticSystemTechniquesTechnologyTrainingValidationWorkage associatedage associated cognitive impairmentage associated memory declineage associated memory deficitage correlatedage dependentage linkedage relatedage related cognitive deficitage related cognitive dysfunctionage related cognitive impairmentage related memory dysfunctionage specificage-associated memory impairmentage-induced cognitive declineage-related decline in cognitionage-related decline in cognitive functionagesaging related cognitive declinedevelop therapyepigenomicsgene manipulationgenetic manipulationgenetically manipulategenetically perturbglobal gene expressionglobal transcription profileimprovedindividual heterogeneityindividual variabilityindividual variationinsightintervention developmentlife spanlifespanliving systemlong-term memorymembermemory declinenervous system functionneurodevelopmental diseaseneurological diseaseneuronalnew drug treatmentsnew drugsnew pharmacological therapeuticnew therapeuticsnew therapynext generation therapeuticsnovel drug treatmentsnovel drugsnovel pharmaco-therapeuticnovel pharmacological therapeuticnovel therapeuticsnovel therapypathwaypreservationpreventpreventingprimary degenerative dementiaresponsesenile dementia of the Alzheimer typespatial RNA sequencingspatial and temporalspatial gene expression analysisspatial gene expression profilingspatial resolved transcriptome sequencingspatial temporalspatial transcriptome analysisspatial transcriptome profilingspatial transcriptome sequencingspatial transcriptomicsspatially resolved transcriptomicsspatio transcriptomicsspatiotemporalsynapsetherapy developmenttranscriptometreatment developmentvalidations
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Full Description

Project Summary
One of the most crucial functions of an organism's nervous system is the ability to form long-term memories.

However, the molecular mechanisms underlying long-term memory formation have yet to be fully elucidated,

due to the fact that memory is a complex process requiring a coordinated response across multiple neuron

types and brain regions. Moreover, it is unknown how these essential memory components contribute to

variability in individual memory performance, which is particularly prominent in the context of age-related

memory loss. Identifying the molecules involved in these processes is important not only to gain insight into

normal brain function but can also lead to an understanding of disease states such as age-related cognitive

decline, neurodevelopmental disorders, and Alzheimer's disease. A major barrier to identifying the molecular

regulators of long-term memory is the sheer complexity of the mammalian nervous system; therefore, we

propose to use the invertebrate model C. elegans, in which all neurons and synaptic connections in the

organism are already known, to molecularly “define memory.” Here we propose to combine a number of

cutting-edge techniques with behavior in this simple system to generate the most precise snapshot to date of

the nervous system-wide molecular changes that are necessary for memory formation. In Project 1, we will

combine behavioral training, spatial transcriptomics, new techniques that we have developed to simultaneously

profile transcriptomes of somatic and synaptic subcompartments, and temporally and spatially precise gene

manipulation to reveal the most complete molecular snapshot of mechanisms necessary for memory formation

to date. In Project 2, we will use unbiased behavioral profiling to uncover strategies of variability in memory

performance, which we will used to predict individuals likely to exhibit improved memory performance with age.

We will then use epigenomics and genomics techniques to determine which essential memory components

may regulate individual memory performance, followed by functional validation in the context of age-related

memory loss. Combined, the proposed work will not only advance our understanding of one of the fundamental

questions in the field of neuroscience but will also reveal new pathways that may be disrupted in neurological

disorders, along with new targets for the development of therapies that prevent disrupted memory due to

neurological disease.

Grant Number: 4DP2NS132372-02
NIH Institute/Center: NIH

Principal Investigator: Rachel Arey

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