Theoverallgoalofthisproposalistocomparevascularmarkersbetweenamnesticmildcognitiveimpairment(MCI) subjectswithamyloidorAlzheimer?sdisease(AD)pathology,andthenewlyidentifiedMCIsubjectswithsuspected non-amyloidpathology(SNAP-MCI).Theinnovationofthisworkisthatwewillexplorevascularpathologyandits roleasadriverofcognitivedeficitsinthisnewcohort.ComparedtotheamyloidpositiveMCIsubjects,SNAP-MCI subjectsshowsimilarneurodegeneration,similaramnesticsymptoms,butnormalamyloidaccumulationinthebrain. The higher burden of white matter hyperintensities in SNAP-MCI suggests vascular involvement in the disease mechanism.However,notmuchisknownregardingvascularabnormalitiesinthisgroup.Toaddressthisgap,we will compare cerebral blood flow (Aim 1) and cerebrovascular reserve (Aim 2) between cognitively normal older adults,amyloidpositiveMCIsubjects,andSNAP-MCIsubjectsfromtheUniversityofWashingtonADResearch Center(directedbyprimarymentor,Grabowski).Wewillthenrepeatthesemeasurementsafter18-24monthsto tracklongitudinalchanges(Aim3).Wewillassesstheco-localizationofthevascularandamyloidpathologiesusing amyloidpositronemissiontomography(PET,TrainingAim4).WehypothesizethatamyloidpositiveMCIsubjects will have the lowest cerebral blood flow and vascular reserve due to the dual effects of amyloid and neurodegeneration.Importantly,thepresenceofvascularpathologyinSNAP-MCIsubjectswillunderlinetheroleof a non-amyloid, vascular mechanism initiating dementia of Alzheimer type. We will apply arterial spin labeling magnetic resonance imaging (MRI) to estimate cerebral blood flow. We will use a breath-hold functional MRI paradigm,validatedinourlab,toevaluatecerebrovascularreserve.InasubsetofMCIsubjects,wewillperform dynamicPETimagingtodetermineR1,i.e.,PETmeasureofCBF,andcorrelateitwithourMRImeasureofCBF. WewillusethestaticFlorbetapir18FPETimagesforasemi-quantitativeregionalanalysisofamyloidaccumulation. Thesignificanceofthisworkisthatitwillenableustoidentifyvasculartargetsforearlyintervention.Ourfuturework willfocusonapplyingtauPETtodetermineneurodegenerationpatternsthatarespecifictoSNAP-MCIandtheir relationtovascularabnormalities.Candidate:Thelong-termgoalofthecandidateistobecomealeaderinAD imagingresearch.ThecandidatehasastrongtechnicalbackgroundinMRIphysics,dataprocessing,andanalyses. Shefirmlybelievesthatamulti-modalanalysisisthekeytobridgethesystems-levelMRImarkerswiththecellular levelPETmarkersforabetterunderstandingofADmechanisms.Tocomplementhertechnicalbackground,she willtakecoursesinneurology,allowinghertoformulateandtestwell-informedhypothesesfordegenerativedisease mechanisms.ShewillsecurenewskillsinstaticanddynamicPETanalyses,aswellasPET-MRIimagefusion.She hasprovidedadetailedplanforherresearchpublicationsandfirstR01submission.Thecandidate?smentorswill ensurethatsheiswell-preparedtolaunchherindependentcareerasanimagingresearchscientist.

Public Health Relevance

The overall goal of this proposal is to identify vascular MRI biomarkers that distinguish heterogeneous MCI populationsatriskofAlzheimer?sDisease(AD).Concurrenceofcerebralbloodflowandvascularreservedeficits, measuredusingMRI,willbeassessedwithamyloidaccumulationandamyloidtracerkineticsusingFlorbetapir18F PET.Successfulcompletionofthisworkwillprovideaninsightintothephysiologicalmechanismsunderlyingvascular pathologyinAD,andallowdevelopmentofalternativetherapeuticstoarrest,slow,orevenreversediseaseprocesses inAD.

Agency
National Institute of Health (NIH)
Institute
National Institute on Aging (NIA)
Type
Research Scientist Development Award - Research & Training (K01)
Project #
5K01AG055669-03
Application #
9663869
Study Section
Neuroscience of Aging Review Committee (NIA)
Program Officer
Hsiao, John
Project Start
2017-04-01
Project End
2022-03-31
Budget Start
2019-04-01
Budget End
2020-03-31
Support Year
3
Fiscal Year
2019
Total Cost
Indirect Cost
Name
University of Washington
Department
Radiation-Diagnostic/Oncology
Type
Schools of Medicine
DUNS #
605799469
City
Seattle
State
WA
Country
United States
Zip Code
98195
Rane, Swati; Koh, Natalie; Boord, Peter et al. (2018) Quantitative cerebrovascular pathology in a community-based cohort of older adults. Neurobiol Aging 65:77-85