grant

Stress, Weathering, and Blood-Based Biomarkers of Alzheimer’s Disease

Organization UNIVERSITY OF GEORGIALocation ATHENS, UNITED STATESPosted 1 Jun 2022Deadline 31 May 2027
NIHUS FederalResearch GrantFY2025A β-42A β42A-beta 42A-beta42AD dementiaAD related dementiaADRDAPOE e4APOE-ε4APOEε4Abeta-42Abeta42AccelerationAccountingAfrican AmericanAfrican American groupAfrican American individualAfrican American peopleAfrican American populationAfrican AmericansAfro AmericanAfroamericanAgeAgingAlcohol DrinkingAlcohol consumptionAlzheimer Type DementiaAlzheimer beta-ProteinAlzheimer disease dementiaAlzheimer sclerosisAlzheimer syndromeAlzheimer'sAlzheimer's Amyloid beta-ProteinAlzheimer's DiseaseAlzheimer's amyloidAlzheimer's and related dementiasAlzheimer's biomarkerAlzheimer's dementia and related dementiaAlzheimer's dementia or related dementiaAlzheimer's disease and related dementiaAlzheimer's disease and related disordersAlzheimer's disease biological markerAlzheimer's disease or a related dementiaAlzheimer's disease or a related disorderAlzheimer's disease or related dementiaAlzheimer's disease related dementiaAlzheimers DementiaAlzheimer’s biological markerAlzheimer’s disease biomarkerAmentiaAmyloidAmyloid Alzheimer's Dementia Amyloid ProteinAmyloid Beta-PeptideAmyloid Protein A4Amyloid SubstanceAmyloid beta-42Amyloid beta-ProteinAmyloid beta42Amyloid βAmyloid β-42Amyloid β-PeptideAmyloid β-ProteinAmyloid β42Amyloidβ-42Amyloidβ42AssayAstrocytesAstrocytusAstrogliaAstroproteinAβ-42Aβ42BMIBMI percentileBMI z-scoreBioassayBiologic ModelsBiologicalBiological AssayBiological MarkersBiological ModelsBloodBlood GlucoseBlood Reticuloendothelial SystemBlood SampleBlood SugarBlood specimenBody mass indexC-reactive proteinCardiovascular DiseasesCausalityChronicChronic DiseaseChronic IllnessChronic stressClinicalCognitionDataDementiaDevelopmentDiabetes MellitusDietDifferences between sexesDiffers between sexesDiseaseDisorderEconomic IncomeEconomical IncomeEconomicsEducationEducational aspectsEtOH drinkingEtOH useEtiologyExerciseExposure toFamilyFamily and Community Health StudyFosteringFreezingGFA-ProteinGFAPGeneralized GrowthGenerationsGeneticGenetic RiskGlial Fibrillary Acid ProteinGlial Fibrillary Acidic ProteinGlial Intermediate Filament ProteinGlycohemoglobin AGlycosylated hemoglobin AGrimAge clockGrowthHannum clockHb A1Hb A1a+bHb A1cHbA1HbA1cHealthHemoglobin A(1)Horvath clockIllness impactImpoverishedIncomeIndividualInflammationInterceptInvestigationInvestigatorsKidney DiseasesLife StyleLifestyleLightMeasuresMediatingModel SystemModelingNational Institute of AgingNational Institute on AgingNational Institutes of HealthNatureNephropathyNerve DegenerationNeuron DegenerationNon-HispanicNonhispanicNot Hispanic or LatinoObservation researchObservation studyObservational StudyObservational researchParticipantPathologic ProcessesPathological ProcessesPathologyPathway interactionsPatient Self-ReportPatternPersonsPhenoAge clocksPhotoradiationPhysiologicPhysiologicalPopulationPovertyPrimary Senile Degenerative DementiaProteins, specific or class, C-reactiveQuetelet indexReligionRenal DiseaseResearchResearch PersonnelResearchersRisk FactorsSamplingSampling StudiesSelf-ReportSex DifferencesSexual differencesSmokingSocial supportStressTestingTimeTissue GrowthUnited States National Institutes of HealthUniversitiesa beta peptideabetaaccelerated agingaccelerated biological ageaccelerated biological agingage accelerationage associated biomarkersage associated markerage clockage markerage related biomarkersage related markersagesaging clocksalcohol ingestionalcohol intakealcohol product usealcohol usealcoholic beverage consumptionalcoholic drink intakeamyloid betaamyloid-b proteinapo E-4apo E4apo epsilon4apoE epsilon 4apoE-4apoE4apolipoprotein E epsilon 4apolipoprotein E-4apolipoprotein E4astrocytic gliabeta amyloid fibrilbio-markersbiologicbiologic markerbiological markers of agebiomarkerbiomarkers of ageblood-based biomarkerblood-based markercardiovascular disordercaucasian Americancausationchildhood adversitychronic disorderclock measuring biological ageclock measuring biological agingclock of biological agingcommunity level disadvantageconferenceconventioncytokinedevelopmentaldiabetesdietsdisadvantaged communitydisease causationdisparity in healtheconomicepigenetic age clocksepigenetic clockepigenetic molecular clocksethanol consumptionethanol drinkingethanol ingestionethanol intakeethanol product useethanol usehazardhealth disparityhemoglobin A1cincomesinflammation markerinflammatory markerinterestkidney disorderlife-style factorlifestyle factorsmedical collegemedical schoolsmethylation clockmethylomicsneighborhood barrierneighborhood disadvantageneighborhood-level barrierneighborhood-level disadvantageneural degenerationneurodegenerationneurodegenerativeneurofilamentneurological degenerationneuronal degenerationontogenyp-taup-τpace of agingpace of biological agingpathwaypediatric adversityphospho-tauphospho-τphosphorylated taupolygenetic risk scorespolygenic risk scorepost-translational modification of tauposttranslational modification of taupredictive biological markerpredictive biomarkerspredictive markerpredictive molecular biomarkerprimary degenerative dementiapsychosocialpsychosocial well-beingpsychosocial wellbeingpsychosocial wellnessrate of agingrate of biological agingreligiousrenal disorderresilience factorresiliency factorschool of medicinesenile dementia of the Alzheimer typesexsex based differencessex-dependent differencessex-related differencessex-specific differencessocialsocial support networksoluble amyloid precursor proteinspeed of agingspeed of the agingstressorsummitsymposiasymposiumtau phosphorylationtau posttranslational modificationtau-1vectorwhite Americanτ phosphorylation
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Full Description

Worldwide, over 50 million people have dementia, with Alzheimer’s disease (AD) accounting for as much as 70% of all cases. Recently, the NIA in conjunction with the Alzheimer’s Association has proposed a biological definition of AD based on the underlying pathological processes of amyloid (A), phosphorylated tau (T), and neurodegeneration (N). Notably, blood-based biomarkers of AT(N) are now available for use in observational studies and for clinical utilization. Unfortunately, African Americans have rarely been included in studies of AD or investigations of the AT(N) framework. This omission is critical given that they are at least twice as likely as
whites to develop AD and evidence suggests that the nature of the pathology (mixed versus pure AD) and the pathways to onset may be quite different for African Americans. The proposed research will use the Family and Community Health Study (FACHS), a unique 25-year ongoing study of physical and psychosocial well-being among several hundred families, to investigate the extent to which a variety of social and economic stressors, lifestyle and genetic factors, rate of aging, and chronic illness impact trajectories of AT(N) biomarkers. The few extant African American dementia studies use samples with higher income and education than the general
African American population. In contrast, the FACHS sample contains a substantial proportion of individuals who have faced the challenges of economic hardship and low education chronic stressors for most of their lives. Our team of investigators from the University of Georgia and Wake Forest University School of Medicine will begin by performing assays of AT(N) biomarkers using frozen blood samples drawn in 2008 and 2019, as well as a new round of blood samples to be obtained in 2024. These data will enable us to use growth curves with individually varying time points (age) to estimate developmental trajectories of AT(N) biomarkers. Next, we will investigate the unique contributions of various environmental, lifestyle, and biological/physiological factors in accelerating these AT(N) trajectories. We are especially interested in testing models where biological/physiological markers of health serve to mediate or moderate the effect of lifestyle and environmental circumstances on changes in AT(N) biomarkers.

Grant Number: 4R01AG077386-02
NIH Institute/Center: NIH
Principal Investigator: Steven Beach

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