grant

Understanding Biological and Lifestyle Contributions to Alzheimer's Disease Pathology and Clinical Profiles in Black Women: Defining Prevention Targets in High Risk Groups

Organization UNIVERSITY OF CALIFORNIA, SAN DIEGOLocation LA JOLLA, UNITED STATESPosted 15 Dec 2022Deadline 30 Nov 2027
NIHUS FederalResearch GrantFY2026(TNF)-α21+ years oldAD biological markerAD biomarkerAD dementiaAD pathologyAD related biomarkerAD riskAD risk factorAdultAdult HumanAdverse effectsAlzheimer Type DementiaAlzheimer disease dementiaAlzheimer risk factorAlzheimer sclerosisAlzheimer syndromeAlzheimer'sAlzheimer's DiseaseAlzheimer's biomarkerAlzheimer's disease biological markerAlzheimer's disease biomarkerAlzheimer's disease pathologyAlzheimer's disease related biomarkerAlzheimer's disease riskAlzheimer's pathologyAlzheimer's related biomarkerAlzheimers DementiaAlzheimer’s biological markerAmentiaAreaAutomobile DrivingB cell differentiation factorB cell stimulating factor 2B-Cell Differentiation FactorB-Cell Differentiation Factor-2B-Cell Stimulatory Factor-2BCDFBSF-2BSF2BehavioralBiologic FactorBiologicalBiological FactorsBiological MarkersBlackBlack AmericanBlack PopulationsBlack groupBlack individualBlack peopleBlack raceBlacksBloodBlood PlasmaBlood Reticuloendothelial SystemCD 120b AntigenCD120b AntigensCachectinCaucasian FemalesCaucasian WomenCaucasian maleCaucasian menCell Communication and SignalingCell SignalingCharacteristicsClinicalCognitionCognitiveCognitive DisturbanceCognitive ImpairmentCognitive declineCognitive function abnormalCommunitiesCoupledDataDecision MakingDementiaDepositDepositionDiabetes MellitusDiseaseDisorderDisparitiesDisparityDisturbance in cognitionExclusionFemaleGoalsHPGFHealthHealth InequityHepatocyte-Stimulating FactorHigh Risk WomanHybridoma Growth FactorIFN-beta 2IFNB2IL-6IL6 ProteinImmune responseImpaired cognitionInequalities in HealthInequities in HealthInflammationInsulin ResistanceInsulin Resistance PathwayInterleukin-6Intracellular Communication and SignalingLife StyleLifestyleLinkLongitudinal observational studyLos AngelesMGI-2MT-bound tauMacrophage-Derived TNFMeasuresMediatingModificationMonocyte-Derived TNFMyeloid Differentiation-Inducing ProteinNon-HispanicNonhispanicNot Hispanic or LatinoOutcomePETPET ScanPET imagingPETSCANPETTParticipantPathologicPathway interactionsPerimenopausalPerimenopausePhysical activityPilot ProjectsPlasmaPlasma SerumPlasmacytoma Growth FactorPlayPopulationPositron Emission Tomography Medical ImagingPositron Emission Tomography ScanPositron-Emission TomographyPre-DMPrediabetesPrediabetes syndromePrediabetic StatePredispositionPrevalencePreventative strategyPreventionPrevention strategyPreventive strategyPrimary Senile Degenerative DementiaProspective StudiesRaceRacesRad.-PETReceptor ProteinReceptors, Tumor Necrosis Factor, Type IIRegistriesReportingResearchReticuloendothelial System, Serum, PlasmaReversal of Insulin Resistance by LeptinRisk FactorsRisk ReductionRoleSignal TransductionSignal Transduction SystemsSignalingSiteSusceptibilityTNFTNF ATNF AlphaTNF geneTNF-R2TNF-RIITNF-αTNFATNFBRTNFR p75TNFR2TNFR80TNFRSF1BTNFRSF1B ReceptorTNFRSF1B geneTNFαTau forming aggregatesTauopathiesTimeTumor Necrosis FactorTumor Necrosis Factor Beta ReceptorTumor Necrosis Factor Receptor 2Tumor Necrosis Factor Receptor 75Tumor Necrosis Factor Receptor Type 2Tumor Necrosis Factor-alphaVulnerable PopulationsWhite FemalesWhite WomenWomanWomen's studyWorkaberrant tauaberrant tau proteinabnormal tauabnormal tau proteinabnormally aggregated tau proteinadulthoodaggregation in taualzheimer riskat-risk femalesat-risk womenbio-markersbiologicbiologic markerbiological signal transductionbiomarkerbiomarker in ADbiomarker in Alzheimer'sbiomarker in Alzheimer's diseasebiopsychosocialblack femaleblack womenblood-based biomarkerblood-based markercaucasian Americancognitive dysfunctioncognitive functioncognitive losscognitive performancecohortcohort investigationcohort researchcommunity advisory boardcommunity advisory committeecommunity advisory panelcommunity based participatory researchcommunity led researchcommunity participatory researchcommunity partnered participatory researchcommunity partnershipcomparing females and malescomparing women and mendeprivationdiabetesdifferences due to racedifferences in racediffers by racediffers in racedisparities in racedisparities in sexdisparity due to racedisparity in healthdrivingexperiencefemale outcomesfemale studyfemales at high riskfemales compared to malesfemales compared with malesfemales versus malesfemales vs. malesfilamentous tau inclusionhealth disparityhealth inequalitieshigh riskhigh risk femaleshigh risk grouphigh risk individualhigh risk peoplehigh risk populationhost responseimmune system responseimmunoresponseindexinginequality due to raceinequity due to raceinflammation markerinflammatory markerinsulin resistantinsulin sensitivityinsulin toleranceinterestinterferon beta 2investigate cohortlife-style factorlifestyle factorslong term observational studylow SESlow socio-economic positionlow socio-economic statuslow socioeconomic positionlow socioeconomic statusmalleable riskmenmenopause transitionmicrotubule associated protein tau aggregationmicrotubule associated protein tau depositmicrotubule associated protein tau mutationmicrotubule bound taumicrotubule-associated protein tau mutationmicrotubule-bound taumodifiable riskmutant taumutant tau proteinmutation in microtubule associated protein taumutation in microtubule-associated protein tauneural inflammationneuroinflammationneuroinflammatoryneuropathologic tauneuropathological tauolder adultolder adulthoodolder womenoutcomes among femalesoutcomes among womenoutcomes in femalesoutcomes in womenp-taup-τpaired helical filament of tauparticipatory action researchpathogenic taupathogenic tau gene mutationpathogenic tau proteinpathological change in taupathological taupathological tau proteinpathwayperi-menopausalperi-menopausephospho-tauphospho-τphosphorylated taupilot studypositron emission tomographic (PET) imagingpositron emission tomographic imagingpositron emitting tomographypost-translational modification of tauposttranslational modification of taupre-diabetespre-diabeticprediabeticpreventpreventingprimary degenerative dementiaprospective research studyprospective surveyprotective factorsrace based differencesrace based disparityrace based inequalityrace based inequityrace differencesrace disparityrace related differencesrace related disparityrace related inequalityrace related inequityracialracial backgroundracial differenceracial disparityracial inequalityracial inequityracial originracially differentracially unequalreceptorrecruitreduce 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-reducingself-aggregate tausenile dementia of the Alzheimer typesexsex disparitysocial determinantssocial health determinantssocial rolesociodeterminantstudy among femalesstudy among womenstudy cohortstudy in femalesstudy in womenstudy on femalesstudy on womenstudy within womensurvey cohorttautau PHFtau Proteinstau abnormalitytau accumulationtau aggregatetau aggregationtau associated neurodegenerationtau associated neurodegenerative processtau driven neurodegenerationtau factortau fibrillationtau fibrillizationtau filamenttau inclusiontau induced degenerationtau induced neurodegenerationtau intronic mutationtau mediated neurodegenerationtau mutationtau neurodegenerative diseasetau neurofibrillary tangletau neuropathologytau oligomertau paired helical filamenttau pathological changetau pathologytau pathophysiologytau phosphorylationtau polymerizationtau posttranslational modificationtau protein accumulationtau protein aggregationtau proteinopathytau related neurodegenerationtau-1tau-induced pathologytau-tau interactiontauopathic neurodegenerative disordertauopathytransition to menopausetransitional menopausetumor necrosis factor receptor superfamily, member 1Bvulnerable groupvulnerable individualvulnerable peoplewhite Americanwhite malewhite menwomen at high riskwomen compared to menwomen compared with menwomen versus menwomen vs. menwomen's outcomesτ Proteinsτ aggregationτ mutationτ phosphorylation
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Full Description

PROJECT SUMMARY/ABSTRACT
Women have higher rate of Alzheimer's disease (AD) and tend to show a more aggressive profile of AD than

men, with greater pathological tau burden and steeper cognitive decline. The prevalence of AD also differs by

race with higher rates among Black versus White older adults. Yet, very little is known about AD in Black

individuals given their historical exclusion in research. Even less is known about the intersection of race and sex

in AD. In this proposal, we aim to study how sex- and/or race-disparate biological (inflammation, insulin resistance

[IR]) pathways and physical activity potentially contribute to tau accumulation and cognitive decline specifically

among older Black women at-risk for AD. We focus on potentially modifiable risk/protective factors given the

recent surge in evidence that modification of these factors can be highly effective in delaying or even preventing

cognitive decline. Our own preliminary work indicated that women may be more susceptible than men to the

adverse effect of inflammation on levels of phosphorylated tau (p-tau) and cognitive function. There is also

evidence that certain lifestyle factors, including physical activity, have a greater impact on AD-related outcomes

such as tau in women versus men. Given links between physical activity and inflammation, we propose to

investigate the interplay between inflammation and physical activity in their contributions to tau and cognitive

decline in older Black women at risk for AD. Since IR is a key driver of inflammation, and the rates of

prediabetes/diabetes are higher in Black adults, we will examine how IR impacts tau accumulation and cognitive

decline. It is critical to examine these relationships in the context of social determinants of health, which are a

driving factor in health outcomes such as inflammation and IR particularly in Black women. To achieve this, we

propose a prospective study that will assess all variables of interest and their interactive pathways. The proposed

study will build upon an ongoing pilot study that will collect these variables in 30 White women by study end

(June, 2022), but will represent a more targeted and less invasive study in order to enhance recruitment in the

understudied yet higher risk group of older Black women. We propose to recruit Black women at two sites, one

leveraging an existing research registry of Black women in Los Angeles, and the other leveraging local

community connections and previous research experience to create a new cohort in San Diego. We will use a

community-based participatory research approach to recruitment that involves decision making at each level

involving a Community Advisory Board. We will measure inflammatory markers in blood, IR, physical activity and

the Area Deprivation Index as our primary social determinant of interest in 100 Black women at-risk for AD and

relate these measures to changes in cognitive function and accumulation of tau, measured in plasma, over a

two-year period. This project will help to close critical gaps in our understanding of risk factors for AD in Black

women by examining biomarkers and social determinants of health in this under-researched yet highly-

vulnerable group. Furthermore, our findings will inform risk reduction strategies that influence these mechanisms.

Grant Number: 3R01AG077579-04S1
NIH Institute/Center: NIH

Principal Investigator: SARAH BANKS

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