Search Existing Data Requests

The Knight ADRC has supported many investigators at Washington University and at other institutions over the years. We wish to avoid the situation where two investigators study the same research question to avoid duplication of effort and potential conflict. To determine if your topic has already been studied with our resources, please search our database. If you find that your topic or a related topic has been submitted, you may wish to contact the investigator to inquire about their findings to determine how you might proceed. You may wish to collaborate or modify your request to avoid overlap. The results below reflect requests made since online requests have been accepted. As such, not all fields will have data as certain information, such as aims, were not collected until recently. If an entry has been assigned an ID number (e.g. T1004), the full request has been submitted and is either approved, disapproved or in process. If an entry has no ID number, then it represents a submission that has not yet been reviewed. Search terms are applied across an entire requests application including variables not displayed below. A more specific, detailed search may yield better results depending upon your needs.


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Investigator: Mony J de Leon

Project Title: CSF clearance in Alzheimer Disease

Date: [153]

Request ID: D1805

Aim 1: CSF clearance in Alzheimer�s disease

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Investigator: Dr. Judy Pa

Project Title: Is CSF sPDGFRβ, a measure of vascular dysfunction, related to functional connectivity among brain regions associated with Alzheimer�s disease

Date: [153]

Request ID: D1804

Aim 1: Determine if vascular impairment affects functional connectivity using rsfMRI data

Aim 2: use DWI data to determine if vascular impairment affects structural connectivity

Aim 3: determine a time line of events, does vascular impairment affect FC first versus SC

Aim 4: explore the relationship between clinical diagnosis, vascular impairment and functional connectivity


Investigator: Isabelle Bos

Project Title: The relationship between dementia risk factors and AD biomarkers in preclinical AD

Date: [153]

Request ID: D1803

Aim 1: investigate the association between AD biomarkers and common risk factors for dementia in cognitively normal individuals and their influence on cognitive decline.

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Investigator: Suzanne Schindler

Project Title: Development of a model for time of amyloid accumulation in Late Onset Alzheimer Disease (LOAD)

Date: [153]

Request ID: D1802

Aim 1: To determine whether the model for change in SUVR as a function of SUVR can be further optimized by incorporating additional covariates (e.g. age, APOE e4 genotype)

Aim 2: To examine how other biomarkers change as a function of amyloid time, including CSF biomarkers, imaging biomarkers (structural brain MRI and tau PET) and cognitive measures.

Aim 3: To create a model for estimated time until dementia onset (EYO) in late onset AD using amyloid time and covariates known to affect risk for dementia, including age, gender, years of education, APOE 4 genotype, race and vascular risk factors.

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Investigator: Lan Tan

Project Title: Genome-wide association study based on A/T/N system identifies new susceptibility loci for Alzheimer�s disease

Date: [153]

Request ID: D1801

Aim 1: We conducted a case-control genome-wide association studies (GWAS) based on �A/T/N� system from 699 participants in Alzheimer�s Disease Neuroimaging Initiative (ADNI) cohort. We want to test our findings in Knight ADRC.

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Investigator: John Morris

Project Title: African American and Caucasian racial difference

Date: [153]

Request ID: D1732

Aim 1: If CMB (cerebral microbleeds) scale (severity and distribution) is jointly analyzed as function of age and race, after adjustment of other covariates, was there any significant difference between the two races?

Aim 2: If WMH (white matter hyperintensities) scale is jointly analyzed as function of age and race, after adjustment of other covariates, was there any significant difference between the two races?

Aim 3: If global amyloid burden (MCBP or MCSUVR) is jointly analyzed as function of age and race, after adjustment of other covariates, was there any significant difference between the two races?

Aim 4: Is there any overall significant difference between the two races in healthy volunteers and the stroke patients


Investigator: Makoto Ishii

Project Title: Alterations in leptin signaling and the hypothalamus in Alzheimer’s disease

Date: [153]

Request ID: D1731

Aim 1: To determine in longitudinal studies if baseline levels of plasma leptin and related metabolic molecules are associated with increased risk of developing: 1) cognitive decline (CDR 0 to 0.5), 2) Alzheimer’s disease diagnosis, or 3) positive biomarkers for Alzheimer’s disease

Aim 2: To determine in longitudinal studies if baseline body weight or body mass index are associated with increased risk of developing: 1) cognitive decline (CDR 0 to 0.5), 2) Alzheimer’s disease diagnosis, or 3) positive biomarkers for Alzheimer’s disease

Aim 3: To determine whether alterations in baseline hypothalamic volume are evident in cognitively intact individuals with positive CSF biomarkers for Alzheimer’s disease

Aim 4: To determine in longitudinal studies if baseline hypothalamic volume are associated with increased risk of developing: 1) cognitive decline (CDR 0 to 0.5), 2) Alzheimer’s disease diagnosis, or 3) positive biomarkers for Alzheimer’s diseas


Investigator: Mark McAvoy

Project Title: Exploring global changes in the brain’s lateralized organization

Date: [153]

Request ID: D1730

Aim 1: Examine the effects of age and dementia status on the brain’s global lateralization

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Investigator: Mark McAvoy

Project Title: Exploring mean global and local BOLD signals in healthy aging and dementia

Date: [153]

Request ID: D1729

Aim 1: Compare the mean global signal with current biomarkers of disease pathology

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Investigator: Yi Su

Project Title: Blood-brain barrier and white matter integrity in aging and dementia

Date: [153]

Request ID: D1728

Aim 1: investigate white matter changes in aging and dementia

Aim 2: investigate blood-brain barrier changes in aging and dementia

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