grant

Midlife Vascular Risk Factors for Alzheimer's Disease in Persons with HFpEF

Organization EMORY UNIVERSITYLocation ATLANTA, UNITED STATESPosted 1 Dec 2022Deadline 30 Nov 2027
NIHUS FederalResearch GrantFY2026(TNF)-α21+ years oldACE2AD biological markerAD biomarkerAD dementiaAD pathwayAD patientsAD related biomarkerAD riskAD risk factorAD-associated pathwaysAD-related pathwaysAD-specific pathwaysAdultAdult HumanAdventitial CellAfrican AmericanAfro AmericanAfroamericanAgeAge YearsAlzheimer Type DementiaAlzheimer beta-ProteinAlzheimer disease dementiaAlzheimer disease mechanismAlzheimer pathwayAlzheimer risk factorAlzheimer sclerosisAlzheimer syndromeAlzheimer'sAlzheimer's Amyloid beta-ProteinAlzheimer's DiseaseAlzheimer's Disease PathwayAlzheimer's amyloidAlzheimer's biomarkerAlzheimer's disease biological markerAlzheimer's disease biomarkerAlzheimer's disease patientAlzheimer's disease related biomarkerAlzheimer's disease riskAlzheimer's mechanismAlzheimer's patientAlzheimer's related biomarkerAlzheimer's related pathwaysAlzheimers DementiaAlzheimer’s biological markerAmyloid (Aβ) plaquesAmyloid Alzheimer's Dementia Amyloid ProteinAmyloid Beta-PeptideAmyloid PlaquesAmyloid Protein A4Amyloid beta-ProteinAmyloid βAmyloid β-PeptideAmyloid β-ProteinAngiotensin Converting EnzymeAngiotensin I-Converting EnzymeArteriesB cell differentiation factorB cell stimulating factor 2B-Cell Differentiation FactorB-Cell Differentiation Factor-2B-Cell Stimulatory Factor-2BBB disruptionBCDFBSF-2BSF2Beta Proprotein Interleukin 1Biological MarkersBlackBlack raceBloodBlood - brain barrier anatomyBlood DiseasesBlood Reticuloendothelial SystemBlood VesselsBlood capillariesBlood-Brain BarrierC-reactive proteinCCL2CCL2 geneCD140b AntigensCD143 AntigensCachectinCarboxycathepsinCardiacCardiac OutputCardiovascularCardiovascular Body SystemCardiovascular DiseasesCardiovascular Organ SystemCardiovascular systemCareer Development AwardsCareer Development Awards and ProgramsCareer Development Programs K-SeriesCerebrospinal FluidCerebrovascular CirculationChemokine, CC Motif, Ligand 2DataDevelopmentDiagnosisDiastolic heart failureDipeptidyl Peptidase ADisease ProgressionDysfunctionEnrollmentEssential HypertensionFunctional disorderFutureGoalsHF with preserved ejection fractionHFpEFHP40HPGFHealth Disparities ResearchHealth disparities related researchHeart VascularHemato-Encephalic BarrierHematologic DiseasesHematological DiseaseHematological DisorderHepatocyte-Stimulating FactorHigh PrevalenceHomolog of Mouse T Cell and Mast Cell Growth Factor 40Hybridoma Growth FactorHypertensionIFN-beta 2IFNB2IL-1 betaIL-1 βIL-1-bIL-1βIL-6IL-9IL1-BetaIL1-βIL1B ProteinIL1F2IL1βIL6 ProteinIL9 ProteinIndividualInflammationInflammatoryInterleukin 1betaInterleukin 9 PrecursorInterleukin-1 betaInterleukin-1βInterleukin-6Interleukin-9InterventionK-AwardsK-Series Research Career ProgramsKininase AKininase IIKnowledgeLVEFLeadLeft Ventricular Ejection FractionLeft Ventricular HypertrophyLightLinkLongitudinal StudiesLongitudinal SurveysMCAFMCP-1MCP1MGI-2MT-bound tauMacrophage-Derived TNFMeasuresMemoryMonocyte Chemoattractant Protein-1Monocyte Chemotactic Protein-1Monocyte Chemotactic and Activating FactorMonocyte Chemotactic and Activating ProteinMonocyte Chemotactive and Activating FactorMonocyte Secretory Protein JEMonocyte-Derived TNFMorbidityMyeloid Differentiation-Inducing ProteinNeuritic PlaquesNeurohormonesNon-HispanicNonhispanicNot Hispanic or LatinoPDGF Receptor βPDGF beta ReceptorPDGF β ReceptorPDGFR betaPDGFR-βParticipantPathogenesisPathologicPathway interactionsPb elementPeptidyl-Dipeptidase APericapillary CellPericytesPerivascular CellPersonsPhotoradiationPhysiologic pulsePhysiopathologyPlasmacytoma Growth FactorPlatelet-Derived Growth Factor Receptor Beta PolypeptidePlatelet-Derived Growth Factor Receptor βPlatelet-Derived Growth Factor beta ReceptorPlayPopulationPreinterleukin 1 BetaPrevalencePrimary Senile Degenerative DementiaProteins, specific or class, C-reactivePulseRaceRacesRelative RisksRenin-Angiotensin SystemResearchResearch Career ProgramRiskRisk ReductionRoleRouget CellsSCYA2SamplingScienceSenile PlaquesSmall Inducible Cytokine A2T-Cell Growth Factor P40T-Cell/Mast Cell Growth Factor p40TNFTNF ATNF AlphaTNF geneTNF-αTNFATNFαTestingTimeTrainingTransforming Growth FactorsTranslational Research EnterpriseTumor Growth FactorsTumor Necrosis FactorTumor Necrosis Factor-alphaVascular DiseasesVascular DisorderVascular Hypertensive DiseaseVascular Hypertensive DisorderVisuospatiala beta peptideabetaabeta accumulationabeta aggregationadulthoodagesaging associated diseaseaging associated disordersaging related diseaseaging related disordersalzheimer riskamyloid betaamyloid beta accumulationamyloid beta aggregationamyloid beta plaqueamyloid β accumulationamyloid β aggregationamyloid-b plaqueamyloid-b proteinangiotensin converting enzyme 2angiotensin converting enzyme IIarterial stiffeningarterial stiffnessartery stiffeningartery stiffnessaβ accumulationaβ aggregationaβ plaquesbeta amyloid fibrilbio-markersbiologic markerbiomarkerbiomarker in ADbiomarker in Alzheimer'sbiomarker in Alzheimer's diseaseblood disorderblood flow in brainblood vessel disorderblood-brain barrier disruptionbloodbrain barrierbloodbrain barrier disruptionbrain blood circulationbrain blood flowcapillarycardiovascular disordercardiovascular riskcardiovascular risk factorcareer developmentcerebral blood flowcerebral circulationcerebral hypoperfusioncerebral spinal fluidcerebrocirculationcerebrovascular blood flowcirculatory systemclinical trial implementationcognitive functioncohortcored plaquecytokinedevelopmentaldifferences due to racedifferences in racediffers by racediffers in racediffuse plaquedisease associated with agingdisease of agingdisorder of agingdisorders associated with agingdisorders related to agingdisparity in healthendothelial dysfunctionenrollenzyme activityexperiencehealth disparities sciencehealth disparityheart failure with preserved ejection fractionheart failure with preserved systolic functionheart outputheavy metal Pbheavy metal leadhigh blood pressurehigh riskhigh risk grouphigh risk individualhigh risk peoplehigh risk populationhyper-phosphorylated tauhyperphosphorylated tauhyperpiesiahyperpiesishypertensive diseasehypertensive disorderidiopathic hypertensionimplementation of clinical trialsimprovedinterferon beta 2later in lifelater lifelong-term studylongitudinal outcome studieslongitudinal research studymechanisms in ADmechanisms in Alzheimer's diseasemicrotubule bound taumicrotubule-bound taumid lifemid-lifemiddle agemiddle agedmidlifemortalityneuroendocrine hormonesneurofibrillary tangle formationneurofilamentneurohormonalnovelolder adultolder adulthoodp-taup-τp40 Cytokinep40 Proteinpathophysiologypathwaypathways associated with ADpathways associated with Alzheimer'spathways contribute to Alzheimer'spathways involved in Alzheimer diseasepathways that contribute to ADpathways that drive ADpathways underlying Alzheimer'spatient living with Alzheimer's diseasepatient suffering from Alzheimer's diseasepatient with Alzheimer'spatient with Alzheimer's diseasepatients with ADphospho-tauphospho-τphosphorylated taupost-translational modification of tauposttranslational modification of taupredictive biological markerpredictive biomarkerspredictive markerpredictive molecular biomarkerpreserved ejection fraction heart failureprimary degenerative dementiaprimary hypertensionrace based differencesrace differencesrace related differencesracialracial backgroundracial differenceracial diversityracial originracially differentracially diversereduce riskreduce risksreduce that riskreduce the riskreduce these risksreduces riskreduces the riskreducing riskreducing the riskrisk factor for developing Alzheimer'srisk factor in Alzheimer'srisk of developing Alzheimer'srisk-reducingsenile dementia of the Alzheimer typesocial rolesoluble amyloid precursor proteinspinal fluidtangle formationtautau Proteinstau factortau phosphorylationtau posttranslational modificationtau-1transforming growth factors Animal growth regulatorstranslation research enterprisetranslational research programvascularvascular dysfunctionvascular risk factorvasculopathyvisual spatialτ Proteinsτ phosphorylation
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Full Description

ABSTRACT
The purpose of this study is to determine the extent to which vascular risk factors are associated with

biomarkers of Alzheimer’s disease (AD) risk over time in middle aged adults with heart failure with preserved

ejection fraction (HFpEF). Mid-life cardiovascular risk factors contribute to the development of AD in later life

and to AD progression. Pathophysiologic mechanisms in HFpEF share mechanistic pathways implicated in AD

development, such as cerebral hypoperfusion, blood brain barrier (BBB) disruption, systemic and central

inflammation, and neurohormonal dysregulation. These AD pathways lead to accumulation of AD biomarkers

in cerebral spinal fluid (CSF) and blood. This study will enroll persons with HFpEF to elucidate vascular risk

factors specific to this understudied population with pathophysiologic drivers of vascular dysfunction associated

with AD risk. The proposed longitudinal study will test the hypothesis that midlife vascular risk factors predict

biomarkers of AD risk in persons with HFpEF. We will test the following Specific Aims in a high-risk cohort of

80 non-Hispanic White (n=40) and Black/African American (n=40) individuals during middle age (45-65yrs)

who have a diagnosis of HFpEF over 2 years: 1) assess the association of vascular risks with CSF biomarkers

of AD risk over two years in middle aged adults with HFpEF, 2) assess the association of vascular risks with

blood biomarkers of AD risk over two years in middle aged adults with HFpEF, and 3) assess the association

of vascular risks with cognitive function over two years in middle aged adults with HFpEF. This career

development award builds on previously developed strengths in studying mechanisms in cardiovascular

disease pathophysiology and aims to fill the gap related to Alzheimer’s disease research in the applicant’s

training. Specific career development goal included in this plan are: 1) gain expertise in the science of AD and

AD biomarkers, including collecting and analyzing AD biomarkers from blood and cerebrospinal fluid and

vascular function measures, 2) gain advanced training and experience in cognitive function measures, 3) gain

expertise in clinical trial implementation, 4) refine knowledge in health disparities research, and 5) transition to

independence and prepare for the next stage of my translational research program. Findings from this study

will lead to the identification of pathways that might be amenable to interventions that improve vascular

function for persons with HFpEF, with the goal of decreasing AD risk in this high morbidity population.

Grant Number: 5K23AG076977-04
NIH Institute/Center: NIH

Principal Investigator: Brittany Butts

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